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EP2310385A2 - Solid pharmaceutical composition - Google Patents

Solid pharmaceutical composition

Info

Publication number
EP2310385A2
EP2310385A2 EP09788017A EP09788017A EP2310385A2 EP 2310385 A2 EP2310385 A2 EP 2310385A2 EP 09788017 A EP09788017 A EP 09788017A EP 09788017 A EP09788017 A EP 09788017A EP 2310385 A2 EP2310385 A2 EP 2310385A2
Authority
EP
European Patent Office
Prior art keywords
give
granules
solid preparation
salt
acid
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Granted
Application number
EP09788017A
Other languages
German (de)
French (fr)
Other versions
EP2310385B1 (en
Inventor
Yutaka Tanoue
Junya Nomura
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Takeda Pharmaceutical Co Ltd
Original Assignee
Takeda Pharmaceutical Co Ltd
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
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Application filed by Takeda Pharmaceutical Co Ltd filed Critical Takeda Pharmaceutical Co Ltd
Publication of EP2310385A2 publication Critical patent/EP2310385A2/en
Application granted granted Critical
Publication of EP2310385B1 publication Critical patent/EP2310385B1/en
Active legal-status Critical Current
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Links

Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/10Dispersions; Emulsions
    • A61K9/12Aerosols; Foams
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D413/00Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and oxygen atoms as the only ring hetero atoms
    • C07D413/14Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and oxygen atoms as the only ring hetero atoms containing three or more hetero rings
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/41Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having five-membered rings with two or more ring hetero atoms, at least one of which being nitrogen, e.g. tetrazole
    • A61K31/4245Oxadiazoles
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P43/00Drugs for specific purposes, not provided for in groups A61P1/00-A61P41/00
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P7/00Drugs for disorders of the blood or the extracellular fluid
    • A61P7/10Antioedematous agents; Diuretics
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/02Non-specific cardiovascular stimulants, e.g. drugs for syncope, antihypotensives
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/08Vasodilators for multiple indications
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/10Drugs for disorders of the cardiovascular system for treating ischaemic or atherosclerotic diseases, e.g. antianginal drugs, coronary vasodilators, drugs for myocardial infarction, retinopathy, cerebrovascula insufficiency, renal arteriosclerosis
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/12Antihypertensives

Definitions

  • the present invention relates to a solid preparation comprising a compound represented by the formula (I) to be shown below, a pH control agent and a diuretic, which is superior in the stability and dissolution property of the compound (I) and the diuretic.
  • a benzimidazole derivative having a strong angiotensin II receptor antagonistic activity which is represented by the formula (I)
  • R 1 is a monocyclic nitrogen-containing heterocyclic group having a deprotonizable hydrogen atom
  • R 2 is an esterified carboxyl group
  • R 3 is an optionally substituted lower alkyl, or a salt thereof (hereinafter sometimes to be referred to as compound (I) ) , particularly (5-methyl-2-oxo- 1, 3-dioxol-4-yl) methyl 2-ethoxy-l- ⁇ [2' - (5-oxo-4, 5-dihydro- 1,2, 4-oxadiazol-3-yl) biphenyl-4-yl]methyl ⁇ -lH-benzimidazole-7- carboxylate salt (patent document 1) , is considered to be a promising therapeutic drug for hypertension and the like.
  • a combination drug product a combination of a compound having an angiotensin II antagonistic activity and a compound having a diuretic action (patent document 2), and an internal solid preparation containing acetaminophen granules obtained by a separating granulation method to suppress the unpleasant taste and prevent discoloration of acetaminophen
  • patent document 1 WO2005/080384 patent document 2: US-B-5721263 patent document 3: JP-A-2001-294524 SUMMARY OF THE INVENTION
  • a preparation containing compound (I) and a diuretic is effective for the prophylaxis or treatment of circulatory diseases such as hypertension, cardiac failure, diabetic nephropathy, arteriosclerosis and the like, and has extremely high clinical usefulness.
  • the problem of the present invention is to provide a solid preparation superior in the stability of compound (I) and a diuretic as well as the dissolution property thereof.
  • the present inventors have conducted intensive studies in an attempt to simultaneously achieve the stability of compound (I) in a preparation and dissolution property thereof from the preparation, and found that the objects can be unexpectedly accomplished by the co-presence of a pH control agent and compound (I), and further, by adjusting, with a pH control agent, the pH range of a solid preparation thereof to a pH range in which the solubility of compound (I) becomes low.
  • a diuretic and compound (I) containing a pH control agent can be further stabilized by separately granulating them, whereby a preparation more superior in the dissolution property of compound (I) as compared to general granulation preparations can be obtained, which resulted in the completion of the present invention.
  • the present invention relates to: [1] a solid preparation comprising a compound represented by the formula (I):
  • R 1 is a monocyclic nitrogen-containing heterocyclic group having a deprotonizable hydrogen atom
  • R 2 is an esterified carboxyl group
  • R 3 is an optionally substituted lower alkyl, or a salt thereof, a pH control agent and a diuretic
  • R 1 is a monocyclic nitrogen-containing heterocyclic group having a deprotonizable hydrogen atom
  • R 2 is an esterified carboxyl group
  • R 3 is an optionally substituted lower alkyl, or a salt thereof and a pH control agent
  • a second part comprising a diuretic, which is obtained by granulating separately from the first part
  • the solid preparation of [1] wherein the compound represented by the formula (I), or a salt thereof and the pH control agent are contained in a first part and the diuretic is contained in a second part, which is a multi-layer tablet comprising a first layer comprised of the first part and a second layer comprised of the second part, [10] the solid preparation of [1], wherein the pH control agent is in a proportion of 0.01-20 wt% of the preparation
  • a method of stabilizing a compound represented by the formula (I) or a salt thereof and a diuretic in a solid preparation which comprises adding a pH control agent to the
  • the solid preparation of the present invention comprising compound (I) , a pH control agent and a diuretic can provide a preparation superior in the stability and dissolution property of compound (I) and the diuretic.
  • Fig. 1 shows dissolution profiles of the tablets obtained in Example 14 and Reference Example 3.
  • Fig. 2 shows dissolution profiles of the tablets obtained in Example 15 and Reference Example 4.
  • the solid preparation of the present invention contains compound (I) , a pH control agent and a diuretic (also referred to as the solid preparation of the present invention) .
  • the solid preparation of the present invention is superior in the stability of compound (I) , and also superior in the dissolution property of the compound (I) . It is also superior in the stability of the diuretic.
  • a 4, 5-dihydro-5-oxo-l,2, 4-oxadiazol-3-yl group includes three tautomers (a', b' and c' ) represented by the formulas:
  • a 1 b 1 c 1 and 4, 5-dihydro-5-oxo-l, 2, 4-oxadiazol-3-yl group includes all of the above-mentioned a' , b' and c' .
  • R 2 is an esterified carboxyl group and, for example, preferably a carboxyl group esterified by lower (Ci_ 4 )alkyl optionally substituted by a substituent selected from a hydroxyl group, an amino group, a halogen atom, lower (C 2 - 6 ) alkanoyloxy (e.g., acetyloxy, pivaloyloxy, etc.), lower (C 4- .- ?
  • cycloalkanoyloxy (lower (Ci- s) alkoxy) carbonyloxy (e.g., methoxycarbonyloxy, ethoxycarbonyloxy, etc.), (lower (C 3 -7) cycloalkoxy) carbonyloxy (e.g., cyclohexyloxycarbonyloxy, etc.), lower (C 1 -4) alkoxy and 5-methyl-2-oxo-l, 3-dioxolen-4-yl (e.g., (5-methyl-2-oxo-l, 3- dioxolen-4-yl)methoxycarbonyl group, 1-
  • R 3 is an optionally substituted lower alkyl, and preferably a lower (d- 5 )alkyl optionally substituted by a substituent selected from a hydroxyl group, an amino group, a halogen atom and a lower (C 1 - 4 ) alkoxy group (preferably lower (C2-3) alkyl; particularly preferably ethyl) .
  • the salt of a compound represented by the formula (I) is, for example, a pharmaceutically acceptable salt.
  • Examples of the salt of a compound represented by the formula (I) include a salt with an inorganic base, a salt with an organic base, a salt with an inorganic acid, a salt with an organic acid, a salt with a basic or acidic amino acid and the like.
  • Preferable examples of the salt with an inorganic base include alkali metal salt such as sodium salt, potassium salt and the like; alkaline earth metal salt such as calcium salt, magnesium salt and the like; aluminum salt, ammonium salt and the like.
  • salts with an organic base include salts with trimethylamine, triethylamine, pyridine, picoline, ethanolamine, diethanolamine, triethanolamine, dicyclohexylamine, N, N' -dibenzylethylenediamine and the like.
  • salts with an inorganic acid include salts with hydrochloric acid, hydrobromic acid, nitric acid, sulfuric acid, phosphoric acid and the like.
  • the salt with an organic acid include salts with formic acid, acetic acid, trifluoroacetic acid, fumaric acid, oxalic acid, tartaric acid, maleic acid, citric acid, succinic acid, malic acid, methanesulfonic acid, benzenesulfonic acid, p-toluenesulfonic acid and the like.
  • Preferable examples of the salt with a basic amino acid include salts with arginine, lysine, ornithine and the like, and preferable examples of salts with acidic amino acid include salts with aspartic acid, glutamic acid and the like.
  • a salt of (5-methyl-2-oxo-l, 3-dioxol-4-yl) methyl 2- ethoxy-l- ⁇ [2' - (5-oxo-4, 5-dihydro-l, 2, 4-oxadiazol-3- yl) biphenyl-4-yl]methyl ⁇ -lH-benzimidazole-7-carboxylate is preferable, and (5-methyl-2-oxo-l, 3-dioxol-4-yl)methyl 2- ethoxy-l- ⁇ [2' - (5-oxo-4, 5-dihydro-l, 2, 4-oxadiazol-3- yl ) biphenyl-4-yl] methyl ⁇ -lH-benzimidazole-7-carboxylate potassium salt is particularly preferable.
  • the salt of a compound represented by the formula (I) ' may ⁇ be hydrate or non-hydrate.
  • Compound (I) may be a solvate including hydrate or a non- solvate .
  • Compound (I) is preferably in the form of a crystal, and preferably has a melting point of 100 - 250 0 C, particularly 120 - 200 0 C, especially 130 - 180 0 C. [0018] Compound (I) is contained in the solid preparation of the present invention in a proportion of 0.1 - 60 wt%, preferably 1 - 40 wt%, more preferably 5 - 30 wt%. [0019]
  • the pH control agent to be used in the present invention may be any as long as it simultaneously achieves stability of the preparation of compound (I) and dissolution property of compound (I) from the preparation and is applicable to a pharmaceutical product.
  • plural pH control agents may be used in combination.
  • the pH control agent to be used in the present invention preferably has a pH of about 2 to about 5, preferably about 3 to about 5, more preferably about 3 to about 4.
  • an acidic substance such as tartaric acid, citric acid, lactic acid, fumaric acid, phosphoric acid, malic acid, succinic acid, ascorbic acid, acetic acid, acidic amino acid (e.g., glutamic acid, aspartic acid) and the like, an inorganic salt (e.g., alkali metal salt, alkaline earth metal salt, ammonium salt and the like) of these acidic substances, a salt of such acidic substance with an organic base (e.g., basic amino acid such as lysine, arginine and the like, meglumine and the like), a solvate (e.g., hydrate) thereof and the like are used.
  • the pH control agent simultaneously achieves stability of a diuretic and dissolution property of the diuretic from the preparation.
  • the pH of the pH control agent is measured under the following conditions. To be specific, it is the pH of a solution or suspension obtained by dissolving or suspending a pH control agent in water at 25°C at a concentration of 1 w/v% .
  • the pH control agent to be used in the present invention an acidic substance and a basic substance are combined, and the obtained pH control agent may be adjusted such that the pH of the solution or suspension is about 2 to about 5, preferably about 3 to about 5, more preferably about 3 to about 4, when the combined pH control agent is dissolved or suspended in water at 25°C at a concentration of 1 w/v% .
  • the acidic substance to be used in combination include, in addition to the acidic substances having a pH of about 2 to about 5 mentioned above and salts thereof, strong acids such as hydrochloric acid, sulfuric acid, phosphoric acid and like.
  • Examples of the basic substance to be used in combination include inorganic bases (e.g., sodium hydroxide, potassium hydroxide, sodium carbonate, sodium hydrogen carbonate, magnesium carbonate, calcium carbonate, magnesium oxide, ammonia, synthetic hydrotalcite) , organic bases (e.g., basic amino acid such as lysine, arginine, etc., meglumine, and the like) and the like.
  • inorganic bases e.g., sodium hydroxide, potassium hydroxide, sodium carbonate, sodium hydrogen carbonate, magnesium carbonate, calcium carbonate, magnesium oxide, ammonia, synthetic hydrotalcite
  • organic bases e.g., basic amino acid such as lysine, arginine, etc., meglumine, and the like
  • the pH control agent to be used in the present invention preferably affords a solution having a buffering capacity at pH 2 to 5, such as sodium dihydrogen phosphate, monosodium fumarate, a combination of fumaric acid and sodium ion donor and the like.
  • the pH control agent to be used in the present invention is preferably monosodium fumarate or a combination of fumaric acid and sodium ion donor.
  • fumaric acid and sodium hydroxide may be used in combination.
  • the pH control agent is contained in a proportion of 0.01 - 20 wt%, preferably 0.05 - 10 wt%, more preferably 0.1 - 5 wt%, of the solid preparation. [ 0022 ]
  • diuretic in the present invention examples include xanthine derivatives (e.g., theobromine sodium salicylate, theobromine calcium salicylate etc.), thiazide preparations (e.g., ethiazide, cyclopenthiazide, trichloromethyazide, hydrochlorothiazide, hydroflumethiazide, benzylhydrochlorothiazide, penflutizide, polythiazide, methyclothiazide etc.), antialdosterone preparations (e.g., spironolactone, triamterene etc.), carbonic anhydrase inhibitors (e.g., acetazolamide etc.), chlorobenzenesulfonamide agents (e.g., chlorthalidone, mefruside, indapamide etc.), azosemide, isosorbide, ethacrynic acid, piretanide, bu
  • the diuretic in the present invention also includes salts of the compounds recited as the above-mentioned diuretic.
  • a chlorobenzenesulfonamide agent, a thiazide preparation and the like are preferable, and chlorthalidone, hydrochlorothiazide and the like are more preferable. Especially, chlorthalidone is preferable.
  • the diuretic is contained in the solid preparation in a proportion of generally, 0.1 - 60 wt% (appropriately adjusted so that the total of compound (I) and pH control agent will not exceed 100%), preferably 0.5 - 40 wt%, more preferably 1 - 30 wt%.
  • chlorthalidone (converted into a free form) is contained in a proportion of generally 0.1 - 60 wt%, preferably 0.5 - 40 wt%, more preferably 1 - 30 wt%.
  • Hydrochlorothiazide (converted into a free form) is contained in a proportion of generally 0.1 - 60 wt%, preferably 0.5 - 40 wt%, more preferably 1 - 30 wt%.
  • a preferable form of the solid preparation of the present invention is a preparation wherein compound (I) is (5-methyl- 2-oxo-l, 3-dioxol-4-yl) methyl 2-ethoxy-l- ⁇ [2' - (5-oxo-4, 5- dihydro-1, 2, 4-oxadiazol-3-yl) biph ⁇ nyl-4-yl]methyl ⁇ -lH- benzimidazole-7-carboxylate potassium salt and the diuretic is chlorthalidone . [0025]
  • the solid preparation of the present invention examples include a solid preparation suitable for oral administration such as tablets, granules, fine granules, capsules, pills and the like. Therefore, the embodiments of the solid preparation of the present invention include the following preparations. (1) A solid preparation obtained by mixing and granulating compound (I) , a pH control agent and a diuretic (single granulation preparation) . (2) A solid preparation containing a first part containing compound (I) and a pH control agent, and a second part containing a diuretic, which is obtained by separately granulating the first part and the second part (separating granulation preparation - a single layer tablet) .
  • the solid preparation of the above-mentioned (1) simultaneously achieves dissolution property and stability of compound (I) and a diuretic respectively in and from the preparation thereof by the addition of a pH control agent.
  • the dissolution property and stability of compound (I) and the diuretic are respectively improved further.
  • the solid preparation of the above-mentioned (1) can -be produced by a method known per se (e.g., method described in the Japanese Pharmacopoeia 14 th Edition, General Rules for Preparations) .
  • compound (I) a pH control agent, a diuretic, additives and the like are mixed, a binder is added to the mixture to give granules, a lubricant and the like are added to the granules and the mixture is tableted into a tablet.
  • Granules and fine granules can also be produced by a method similar to that of the tablet.
  • the above-mentioned granules and fine granules are filled in a capsule containing gelatin, hydroxypropylmethylcellulose and the like.
  • an active ingredient and a filler are filled in a capsule containing gelatin, hydroxypropylmethylcellulose and the like.
  • the solid preparation may contain additives conventionally used in the pharmaceutical field.
  • additives conventionally used in the pharmaceutical field.
  • the additive include filler, disintegrant, binder, lubricant, colorant, pH control agent, surfactant, stabilizer, acidulant, flavor, glidant and the like. These additives are used in an amount conventionally employed in the pharmaceutical field.
  • the filler examples include starches such as cornstarch, potato starch, wheat starch, rice starch, partly pregelatinized starch, pregelatinized starch, porous starch and the like; sugar and sugar alcohols such as lactose, fructose, glucose, mannitol (e.g., D-mannitol) , sorbitol (e.g., D-sorbitol) , erythritol (e.g., D-erythritol) , sucrose and the like; anhydrous calcium phosphate, crystalline cellulose, microcrystalline cellulose, glycyrrhiza uralensis, sodium hydrogen carbonate, calcium phosphate, calcium sulfate, calcium carbonate, precipitated calcium carbonate, calcium silicate and the like.
  • starches such as cornstarch, potato starch, wheat starch, rice starch, partly pregelatinized starch, pregelatinized starch, porous starch and the like
  • disintegrant examples include amino acid, starch ? cornstarch, carboxymethylcellulose, calcium carboxymethylcellulose, sodium carboxymethyl starch, carmellose sodium, carmellose calcium, croscarmellose sodium, crospovidone, low-substituted hydroxypropylcellulose, hydroxypropylstarch, sodium carboxymethyl starch and the like.
  • binder examples include crystalline cellulose (e.g., microcrystalline cellulose), hydroxypropylcellulose, hydroxypropylmethylcellulose, polyvinylpyrrolidone, gelatin, starch, gum arabic powder, tragacanth, carboxymethylcellulose, sodium alginate, pullulan, glycerol and the like.
  • the lubricant include magnesium stearate, stearic acid, calcium stearate, talc (purified talc) , sucrose esters of fatty acids, stearyl fumarate monosodium salt and the like.
  • colorant examples include food colors such as Food Color Yellow No. 5, Food Color Red No. 2, Food Color Blue No. 2 and the like, food lake colors, diiron trioxide and the like.
  • surfactant examples include sodium lauryl sulfate, polysorbate 80, polyoxyethylene (160) polyoxypropylene (30) glycol and the like.
  • Examples of the stabilizer include tocopherol, tetrasodium edetate, nicotinic acid amide, cyclodextrins and the like.
  • Examples of the acidulant include ascorbic acid, citric acid, tartaric acid, malic acid and the like.
  • Examples of the flavor include menthol, peppermint oil, lemon oil, vanillin and the like.
  • glidant examples include light anhydrous silicic acid, hydrated silicon dioxide and the like.
  • the above-mentioned additives may be a mixture of two ⁇ or more kinds at an appropriate ratio.
  • the solid preparation of the above-mentioned (2) contains a first part and a second part, which are separately granulated, and can be produced by a method known per se.
  • the first part in the present invention is a part (composition) containing compound (I) and a pH control agent.
  • the amount of the pH control agent to be used in the present invention is preferably 0.01 - 20 parts by weight, preferably 0.05 - 10 parts by weight, more preferably 0.1 - 5 parts by weight, per 100 parts by weight of the above- mentioned first part.
  • the weight ratio of compound (I) to a pH control agent is preferably 1 - 30:1, more preferably 5 - 25:1, more preferably 10 - 20:1.
  • the above-mentioned first part is not limited as long as it has a shape and a size that afford a solid preparation together with the below-mentioned second part.
  • the above-mentioned first part may further contain additives conventionally used in the pharmaceutical field. As the additives, those similar to the aforementioned additives can be used.
  • the above-mentioned first part can be produced by mixing compound (I), a pH control agent and, where necessary, the above-mentioned additives and granulating the mixture according to a method known per se.
  • the above-mentioned first part preferably contains compound (I) (preferably (5-methyl-2-oxo-l, 3-dioxol-4- yl) methyl 2-ethoxy-l- ⁇ [2' - (5-oxo-4, 5-dihydro-l, 2, 4-oxadiazol-)
  • the second part in the present invention is a part
  • composition containing a diuretic.
  • the above-mentioned second part is not limited as long as it has a shape and a size that afford a solid preparation together with the above-mentioned first part .
  • the above-mentioned second part may further contain additives conventionally used in the pharmaceutical field.
  • additives those similar to the aforementioned additives can be used.
  • a diuretic preferably chlorthalidone
  • a filler preferably mannitol and crystalline cellulose
  • a binder preferably hydroxypropylcellulose
  • the above-mentioned second part can be produced by mixing a diuretic and, where necessary, the above-mentioned additives and granulating the mixture according to a method known per se.
  • the amount of the diuretic is preferably 0.1 - 60 parts by weight, more preferably 0.5 - 40 parts by weight, more preferably 1 - 30 parts by weight, per 100 parts by weight of the above-mentioned second part.
  • the weight ratio of the second part to the first part in the solid preparation of the present invention is preferably 0.1 - 10:1, more preferably 0.3
  • a single layer tablet produced by mixing a first part and a second part, which are separately granulated, and further, additives conventionally used in the pharmaceutical field, and then compressing the mixture is also encompassed in the solid preparation of the present invention.
  • a capsule produced by- filling the above-mentioned single layer tablet in a capsule e.g., hydroxypropylmethylcellulose capsule is also encompassed in the solid preparation of the present invention.
  • a capsule produced by directly filling the first part and the second part, which are separately granulated, or together with the above-mentioned additives, in a capsule is also encompassed in the solid preparation of the present invention.
  • the first part and the second part are separately granulated, and the preparation can be produced by compressing independently these parts, or coating one part with the other part.
  • solid preparation of the above- mentioned (3) include [1] coated tablet (A) containing an inner core of the first part and an outer layer of the second part; [2] coated tablet (B) containing an inner core of the second part and an outer layer of the first part; [3] a multilayer tablet containing a first layer of the first part and a second layer of the second part. [0048]
  • the inner core of the first part can be produced by, for example, granulating compound (I) , a pH control agent and, where necessary, additives. After granulation, where necessary, an operation of drying, sieving, compression and the like may be applied.
  • the outer layer of the second part can be produced, for example, by granulating a diuretic (e.g., chlorthalidone or a salt thereof) with additives, as necessary.
  • the coating can be performed, for example, by compression, coating and the like.
  • the additive is preferably a binder and the like.
  • an inactive intermediate layer may be inserted between an inner core and an outer layer to prevent a direct contact.
  • the intermediate layer contains, for example, the following coating base and additives for coating.
  • the intermediate layer preferably contains a water-soluble film coating base and a glidant.
  • coated tablet (B) can be produced in the same manner as in coated tablet (A) except that the second part is used as an inner core and first part is used as an outer layer. [0052]
  • the multi-layer tablet of the present invention comprises a first part containing a compound represented by the formula
  • the multi-layer tablet of the present invention is not particularly limited as long as it is a preparation wherein at least the first layer comprised of the first part and the second layer comprised of the second part are integrally formed.
  • the multi-layer tablet in the present invention may have an inactive intermediate layer between the first layer and the second layer.
  • the adverse influences decreased preservation stability such as time-course decomposition of active ingredients, lowered effectiveness and the like, decreased dissolution stability such as time-course changes in dissolution pattern of active ingredients and the like, and so on
  • the adverse influences decreased preservation stability such as time-course changes in dissolution pattern of active ingredients and the like, and so on
  • the multi-layer tablet can be produced, for example, by the following production steps.
  • Compound (I) and a pH control agent are mixed with additives as necessary, and the obtained mixture is granulated to give the first part. After granulation, operations such as drying, sieving and the like may be performed where necessary. Thereafter, additives are mixed where necessary to give the first layer. Then, a diuretic is granulated with additives as necessary, and the obtained second part is mixed with additives as necessary to give the second layer, which is put on the above-mentioned first layer in layers and compressed (preferably tableted) . To prevent a direct contact of respective layers, an inactive intermediate layer may be inserted between the respective layers.
  • the intermediate layer contains, for example, the above-mentioned filler, disintegrant, binder, lubricant, colorant and the like.
  • a capsule produced by filling the above-mentioned coated tablet (A) or (B) or multi-layer tablet in a capsule (e.g., hydroxypropylmethylcellulose capsule) is also encompassed in the solid preparation of the present invention.
  • a film coating preparation produced by coating the above-mentioned solid preparation (1) - (3) with a film of the following coating base and additives for coating is also encompassed in the solid preparation of the present invention.
  • the coating base include a sugar coating base, a water-soluble film coating base, an enteric film coating base, a sustained-release film coating base and the like.
  • sucrose is used as the sugar coating base.
  • talc precipitated calcium carbonate
  • gelatin gum arabic
  • pullulan a substance selected from a sugar styrene
  • carnauba wax a substance selected from a sugar styrene
  • talc precipitated calcium carbonate
  • gelatin gum arabic
  • pullulan a substance selected from a sugar styrene
  • water-soluble film coating base examples include cellulose polymers such as hydroxypropylcellulose [e.g., grade: L, SL, SL-T, SSL (trade name); Nippon Soda Co., Ltd.], hydroxypropylmethylcellulose [e.g., TC-5 (grade: MW, E, EW, R, RW) (trade name); Shin-Etsu Chemical Co., Ltd.], hydroxyethylcellulose, methylhydroxyethylcellulose and the like; synthetic polymers such as polyvinyl acetaldiethylaminoacetate, aminoalkylmethacrylate copolymer E [Eudragit E (trade name) ] , polyvinylpyrrolidone and the like; polysaccharides such as pullulan and the like, and so on. [0062]
  • hydroxypropylcellulose e.g., grade: L, SL, SL-T, SSL (trade name); Nippon Soda Co., Ltd.]
  • enteric film coating base examples include cellulose polymers such as hydroxypropylmethylcellulose phthalate, hydroxypropylmethylcellulose acetatesuccinate, carboxymethylethylcellulose, cellulose acetate phthalate and the like; acrylic acid polymers such as methacrylic acid copolymer L [Eudragit L (trade name) ] , methacrylic acid copolymer LD [Eudragit L-30D55 (trade name) ] , methacrylic acid copolymer S [Eudragit S (trade name) ] and the like; naturally occurring substance such as shellac and the like, and so on. [0063]
  • sustained-release film coating base examples include cellulose polymers such as ethylcellulose and the like; acrylic acid polymers such as aminoalkylmethacrylate copolymer RS [Eudragit RS (trade name) ] , ethyl acrylate-methyl - methacrylate copolymer suspension [Eudragit NE (trade name) ] and the like, and so on.
  • cellulose polymers such as ethylcellulose and the like
  • acrylic acid polymers such as aminoalkylmethacrylate copolymer RS [Eudragit RS (trade name) ] , ethyl acrylate-methyl - methacrylate copolymer suspension [Eudragit NE (trade name) ] and the like, and so on.
  • the coating additives include light protecting agents such as titanium oxide and the like, glidants such as talc and the like, colorants such as red ferric oxide, yellow ferric oxide and the like; plasticizers such as polyethylene glycol [e.g., macrogol 6000 (trade name)], triethyl citrate, castor oil, polysorbate and the like; organic acids such as citric acid, tartaric acid, malic acid, ascorbic acid and the like; and so on.
  • light protecting agents such as titanium oxide and the like, glidants such as talc and the like, colorants such as red ferric oxide, yellow ferric oxide and the like
  • plasticizers such as polyethylene glycol [e.g., macrogol 6000 (trade name)], triethyl citrate, castor oil, polysorbate and the like
  • organic acids such as citric acid, tartaric acid, malic acid, ascorbic acid and the like; and so on.
  • the solid preparation of the present invention may have a distinguishable embossing or printed letters, or a scored line for division.
  • the solid preparation of the present invention is preferably film-coated from the aspects of easy administration, mechanical strength and the like.
  • the mixing is performed, for example, using a blending machine such as a V-type mixer, a tumbler mixer and the like; and a granulator such as a high speed mixer granulator, a fluid bed granulator, an extrusion-granulator, a roller compactor and the like.
  • a blending machine such as a V-type mixer, a tumbler mixer and the like
  • a granulator such as a high speed mixer granulator, a fluid bed granulator, an extrusion-granulator, a roller compactor and the like.
  • the compression is performed, for example, using a single stroke tableting machine, a rotary tableting machine and the like.
  • a tableting pressure of generally 1 - 20 kN/cm 2 (preferably 5 - 15 kN/cm 2 ) is preferably employed.
  • a taper cutting die is preferably used for preventing capping.
  • the coating is performed, for example, using a film coating apparatus and the like.
  • the solid preparation of the present invention can be used safely as a medicine for mammals (e.g., human, dog, rabbit, rat, mouse and the like) .
  • the daily dose is about 0.05 - 500 mg, preferably 0.1 - 100 mg.
  • the daily dose of a diuretic to patients is determined in consideration of age, body weight, general health condition, sex, diet, administration time, clearance rate, combination of drugs and the like, as well as the severity of the disease for which the patient is undergoing treatments, the daily dose is, for example, about 12.5 - 100 mg, preferably 15 - 50 mg, of chlorthalidone (converted into free form) . In the case of hydrochlorothiazide (converted into free form) , the daily dose is about 12.5 - 100 mg, preferably 15 - 50 mg. [0071]
  • the pharmaceutical composition of the present invention is useful as a prophylactic or therapeutic drug for diseases developed by (or diseases whose onset is promoted by) contraction or growth of blood vessel or an organ disorder expressed via angiotensin II receptor, due to the presence of angiotensin II, or a factor induced by the presence of angiotensin II, in mammals (e.g., human, monkey, cat, swine, horse, bovine, mouse, rat, guinea pig, dog, rabbit and the like) .
  • mammals e.g., human, monkey, cat, swine, horse, bovine, mouse, rat, guinea pig, dog, rabbit and the like.
  • the solid preparation of the present invention is useful as a prophylactic or therapeutic drug for the above-mentioned diseases, can reduce the doses of compound (I) and a diuretic as compared to independent use thereof and can suppress expression of side effects.
  • the present invention provides a method of stabilizing a compound represented by the formula (I) or a salt thereof and a diuretic in a solid preparation containing a compound represented by the formula (I) or a salt thereof, and a diuretic, which includes adding a pH control agent. According to the stabilizing method of the present invention, compound (I) and a diuretic in a solid preparation is significantly stabilized.
  • the present invention provides a method of improving dissolution of a compound represented by the formula (I) or a salt thereof from a solid preparation containing the compound or a salt thereof, and a diuretic, which includes adding a pH control agent. According to the improving method of dissolution property in the present invention, the dissolution property of compound (I) and a diuretic from a solid preparation is significantly improved.
  • Example 1 The present invention is explained in more detail in the following by referring to Examples and Experimental Examples, which are not to be construed as limitative.
  • the components (additives) other than the active ingredient may be those recited in the Japanese Pharmacopoeia, the Japanese Pharmacopoeia Japanese Pharmaceutical Codex or Japanese Pharmaceutical Excipients and the like.
  • compound A 4, 5-dihydro-l, 2, 4-oxadiazol-3-yl) biphenyl-4-yl] methyl ⁇ -IH- benzimidazole-7-carboxylate potassium salt (hereinafter to be referred to as compound A) (1067 g) and mannitol (1968 g) were uniformly mixed, granulated by spraying an aqueous solution of hydroxypropylcellulose (112.5 g) , fumaric acid (46.5 g) and sodium hydroxide (16 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules A.
  • Croscarmellose sodium (24.68 g) , crystalline cellulose (30.86 g) , magnesium stearate (3.08 g) , the sieved granules A (128.4 g) and the sieved granules B (121.5 g) were mixed in a bag to give mixed granules.
  • the mixed granules were tableted by a rotary tableting machine (AQUARIUS, Kikusui Seisakusho, Ltd.) using a 7 mm ⁇ punch (tableting pressure: 4 KN/punch, weight per tablet: 154.26 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 40 0 C for 16 hr.
  • composition of preparation (154.26 mg) compound A 21.34 mg mannitol 39.36 mg hydroxypropylcellulose 2.25 mg fumaric acid 0.93 mg sodium hydroxide 0.32 mg chlorthalidone 25 mg mannitol 33.5 mg hydroxypropylcellulose 2.25 mg croscarmellose sodium 12.34 mg crystalline cellulose 15.43 mg magnesium stearate 1.54 mg total 154.26 mg
  • Croscarmellose sodium (24 g) , crystalline cellulose (30 g) and magnesium stearate (3 g) and the sieved granules A (85.36 g) were mixed in a bag to give mixed granules A.
  • composition of preparation 352.5 mg
  • compound A 85.36 mg mannitol 143.26 mg hydroxypropylcellulose 9 mg fumaric acid 4 mg sodium hydroxide 1.38 mg chlorthalidone 25 mg crystalline cellulose (granules) 18 mg crystalline cellulose 1.5 mg low-substituted hydroxypropylcellulose 4 mg hydroxypropylmethylcellulose 4 mg croscarmellose sodium 24 mg crystalline cellulose 30 mg magnesium stearate 3 mg total 352.5 mg
  • Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I.
  • a fluid bed granulator (WSG-60, POWREX CORPORATION)
  • chlorthalidone 5375 g
  • mannitol 53450 g
  • crystalline cellulose 3870 g
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules A.
  • P-7S Showa Chemical Machinery
  • composition of preparation (280 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg sodium hydroxide 0.345 mg fumaric acid 1 mg hydroxypropylcellulose 2.7 mg crystalline cellulose 27 mg crospovidone 15.75 mg magnesium stearate 2.7 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 280 mg [0080]
  • composition of preparation (280 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg sodium hydroxide 0.345 mg fumaric acid 1 mg hydroxypropylcellulose 2.7 mg crystalline cellulose 27 mg crospovidone 15.75 mg magnesium stearate 2.7 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0 . 06 mg total 280 mg
  • Example 5 Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I.
  • a fluid bed granulator (WSG-60, POWREX CORPORATION)
  • chlorthalidone 5375 g
  • mannitol 53450 g
  • crystalline cellulose 3870 g
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules A.
  • P-7S Showa Chemical Machinery
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules B.
  • (3) Crystalline cellulose (9720 g) , crospovidone (6075 g) , magnesium stearate (972 g) , the milled granules A (40820 g) and the milled granules B (39610 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules .
  • the coating dispersion was sprayed on the core tablets obtained in (4) until the weight of the core tablet increased to 10 mg per tablet to give film-coated tablets having the following composition. Then, the film- coated tablets were dried under the reduced pressure at 40 0 C for 15 hr.
  • composition of preparation (370 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 42.68 mg mannitol 86.93 mg crystalline cellulose 9 mg sodium hydroxide 0.69 mg fumaric acid 2 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 36 mg crospovidone 22.5 mg magnesium stearate 3.6 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 370 mg
  • Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I.
  • a fluid bed granulator (WSG-60, POWREX CORPORATION)
  • chlorthalidone 5375 g
  • mannitol 53450 g
  • crystalline cellulose 3870 g
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules A.
  • P-7S Showa Chemical Machinery
  • composition of preparation (370 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 42.68 mg mannitol 86.93 mg crystalline cellulose 9 mg sodium hydroxide 0.69 mg fumaric acid 2 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 36 mg crospovidone 22.5 mg magnesium stearate 3.6 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 370 mg
  • Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I.
  • a fluid bed granulator (WSG-60, POWREX CORPORATION)
  • chlorthalidone 5375 g
  • mannitol 53450 g
  • crystalline cellulose 3870 g
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules A.
  • P-7S Showa Chemical Machinery
  • the mixed granules were tableted by a rotary tableting machine (AQUARIUS36K, Kikusui Seisakusho, Ltd. ) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10 kN, weight per tablet: 540 mg) to give core tablets.
  • composition of preparation (560 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg hydroxypropylmethylcellulose 15.6 mg talc 2.4 mg titanium oxide 1.88 mg iron oxide 0.12 mg total 560 mg
  • Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I.
  • a fluid bed granulator (WSG-60, POWREX CORPORATION)
  • chlorthalidone (10750 g)
  • mannitol 48070 g
  • crystalline cellulose 3870 g
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules A.
  • P-7S Showa Chemical Machinery
  • the mixed granules were tableted by a rotary tableting machine (AQUARIUS36K, Kikusui Seisakusho, Ltd. ) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10 kN, weight per tablet: 540 mg) to give core tablets.
  • composition of preparation (560 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg hydroxypropylmethylcellulose 15.6 mg talc 2.4 mg titanium oxide 1.88 mg iron oxide 0.12 mg total 560 mg
  • Crystalline cellulose (7200 g) , crospovidone (3600 g) , magnesium stearate (720 g) and the milled granules (60480 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules.
  • Crystalline cellulose (7200 g) , crospovidone (5400 g) , magnesium stearate (720 g) and the milled granules (58680 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules B.
  • Dispersion liquid II and purified water 250 g were added to dispersion liquid I, and the mixture was stirred to give a coating dispersion.
  • a pan coating machine DRC-650, POWREX CORPORATION
  • the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 10 mg per tablet to give film-coated tablets having the following composition. Then, the film-coated tablets were dried under the reduced pressure at 40°C for 15 hr.
  • composition of preparation (280 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 18 mg crospovidone 9 mg magnesium stearate 1.8 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg sodium hydroxide 0.345 mg fumaric acid 1 mg hydroxypropylcellulose 2.7 mg crystalline cellulose 9 mg crospovidone 6.75 mg magnesium stearate 0.9 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 280 mg
  • Hydroxypropylcellulose (5122 g) was dissolved in purified water (80620 g) to give liquid I.
  • a fluid bed granulator (WSG-60, POWREX CORPORATION)
  • chlorthalidone 10740 g
  • mannitol 48080 g
  • crystalline cellulose 3870 g
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules.
  • Crystalline cellulose (7200 g) , crospovidone (3600 g) , magnesium stearate (720 g) and the milled granules (60480 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules.
  • Crystalline cellulose (7200 g) , crospovidone (5400 g) , magnesium stearate (720 g) and the milled granules (58680 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules B.
  • Dispersion liquid II and purified water 250 g were added to dispersion liquid I, and the mixture was stirred to give a coating dispersion.
  • a pan coating machine DRC-650, POWREX CORPORATION
  • the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 10 mg per tablet to give film-coated tablets having the following composition. Then, the film-coated tablets were dried under the reduced pressure at 40 0 C for 15 hr.
  • composition of preparation (280 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 18 mg crospovidone 9 mg magnesium stearate 1.8 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg sodium hydroxide 0.345 mg fumaric acid 1 mg hydroxypropylcellulose 2.7 mg crystalline cellulose 9 mg crospovidone 6.75 mg magnesium stearate 0.9 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 280 mg
  • Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I.
  • a fluid bed granulator (WSG-60, POWREX CORPORATION)
  • chlorthalidone 5375 g
  • mannitol 53450 g
  • crystalline cellulose 3870 g
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules.
  • P-7S Showa Chemical Machinery
  • Crystalline cellulose (7200 g) , crospovidone (3600 g) , magnesium stearate (720 g) and the milled granules (60480 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules.
  • Crystalline cellulose (7200 g) , crospovidone (5400 g) , magnesium stearate (720 g) and the milled granules (58680 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules B.
  • the mixed granules A (180 mg) and the mixed granules B (360 mg) were tableted in the form of a bilayer by a rotary tableting machine (AQUA08242L2JI, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10 kN, weight per tablet: 540 mg) to give core tablets.
  • composition of preparation (560 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 18 mg crospovidone 9 mg magnesium stearate 1.8 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 36 mg crospovidone 27 mg magnesium stearate 3.6 mg hydroxypropylmethylcellulose 15.6 mg talc 2.4 mg titanium oxide 1.88 mg iron oxide 0.12 mg total 560 mg
  • Crystalline cellulose (7200 g) , crospovidone (3600 g) , magnesium stearate (720 g) and the milled granules (60480 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules A.
  • a part of the obtained the granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules.
  • Crystalline cellulose (7200 g) , crospovidone (5400 g) , magnesium stearate (720 g) and the milled granules (58680 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules B.
  • the mixed granules A (180 mg) and the mixed granules B (360 mg) were tableted in the form of a bilayer by a rotary tableting machine (AQUA08242L2JI, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10 kN, weight per tablet: 540 mg) to give core tablets.
  • composition of preparation (560 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 18 mg crospovidone 9 mg magnesium stearate 1.8 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 36 mg crospovidone 27 mg magnesium stearate 3.6 mg hydroxypropylmethylcellulose 15.6 mg talc 2.4 mg titanium oxide 1.88 mg iron oxide 0.12 mg total 560 mg
  • Example 13 (1) In a fluid bed granulator (Lab-1, POWREX CORPORATION), compound A (85.36 g) , chlorthalidone (100 g) , and mannitol
  • composition of preparation (90 mg) compound A 21.34 mg chlorthalidone 25 mg mannitol 22.815 mg hydroxypropylcellulose 2.7 mg fumaric acid 1 mg sodium hydroxide 0.345 mg croscarmellose sodium 6.9 mg crystalline cellulose 9 mg magnesium stearate 0.9 mg total 90 mg
  • Example 14 In a fluid bed granulator (FD-5S, POWREX CORPORATION), compound A (597.5 g) , chlorthalidone (175 g) , mannitol (2000 g) and crystalline cellulose (189 g) were uniformly mixed and granulated by spraying an aqueous solution of hydroxypropylcellulose (113.4 g) , fumaric acid (28 g) and sodium hydroxide (9.66 g) , and dried therein. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules.
  • Crystalline cellulose (324 g) , crospovidone (216 g) , magnesium stearate (32.4 g) and the sieved granules (2668 g) were mixed in a tumbler mixer (TM-15, Showa Chemical Machinery) to give mixed granules.
  • the mixed granules were tableted by a rotary tableting machine
  • composition of preparation (540 mg) chlorthalidone 25 mg compound A 85.36 mg mannitol 285.66 mg crystalline cellulose 27 mg hydroxypropylcellulose 16.2 mg fumaric acid 4 mg sodium hydroxide 1.38 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg total 540 mg [0102]
  • composition of preparation (540 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg hydroxypropylcellulose 10.8 mg fumaric acid 4 mg sodium hydroxide 1.38 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg total 540 mg [0104]
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules B.
  • the mixed granules were tableted by a rotary tableting machine (COLLECT 12K, Kikusui Seisakusho, Ltd.) using a 8.5 mm ⁇ punch (tableting pressure: 6 KN/punch, weight per tablet: 270 mg) to give core tablets.
  • a rotary tableting machine (COLLECT 12K, Kikusui Seisakusho, Ltd.) using a 8.5 mm ⁇ punch (tableting pressure: 6 KN/punch, weight per tablet: 270 mg) to give core tablets.
  • (4) Hydroxypropylmethylcellulose (390 g) and talc (60 g) were dissolved and dispersed in purified water (3850 g) to give dispersion liquid I.
  • Titanium oxide (47 g) and iron oxide (3 g) were dispersed in purified water (500 g) to give dispersion liquid II.
  • Dispersion liquid II and purified water 150 g were added to dispersion liquid I, and the mixture was stirred to give a coating dispersion.
  • a pan coating machine DRC-650, POWREX CORPORATION
  • the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 10 mg per tablet to give film- coated tablets having the following composition. Then, the film-coated tablets were dried under the reduced pressure at
  • composition of preparation (280 mg) chlorthalidone 6.25 mg mannitol 130.55 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg hydroxypropylcellulose 2.7 mg fumaric acid 1 mg sodium hydroxide 0.345 mg crystalline cellulose 27 mg crospovidone 15.75 mg magnesium stearate 2.7 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 280 mg
  • Example 17 (1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I.
  • purified water 44070 g
  • chlorthalidone 2688 g
  • mannitol 5614Og
  • crystalline cellulose 3870 g
  • P-7S Powermill grinder
  • a part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mm ⁇ punching screen to give milled granules B.
  • (3) Crystalline cellulose (1512 g) , crospovidone (1008 g) , magnesium stearate (151.2 g) , the milled granules A (4234 g) and the milled granules B (8215 g) were mixed in a tumbler mixer (TM-60S, Showa Chemical Machinery) to give mixed granules.
  • the mixed granules were tableted by a rotary tableting machine (COLLECT 12K, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10.5 KN/punch, weight per tablet: 540 mg) to give core tablets having the following composition.
  • (4) Hydroxypropylmethylcellulose (390 g) and talc (60 g) were dissolved and dispersed in purified water (3850 g) to give dispersion liquid I. Titanium oxide (47 g) and iron oxide (3 g) were dispersed in purified water (500 g) to give dispersion liquid II.
  • Dispersion liquid II and purified water 150 g were added to dispersion liquid I, and the mixture was stirred to give a coating dispersion.
  • a pan coating machine DRC-650, POWREX CORPORATION
  • the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 20 mg per tablet to give film- coated tablets having the following composition. Then, the film-coated tablets were dried under the reduced pressure at 40°C for 15 hr.
  • composition of preparation (560 mg) chlorthalidone 6.25 mg mannitol 130.55 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5 . 4 mg hydroxypropylmethylcellulose 15 . 6 mg talc 2 . 4 mg titanium oxide 1 . 88 mg iron oxide 0 . 12 mg total 560 mg [0108] Reference Example 1
  • the sieved granules (16.2 g) and low- substituted hydroxypropylcellulose (0.8 g) were mixed in a glass bottle to give mixed granules.
  • the mixed granules were tableted by Autograph (manufactured by Shimadzu Corporation, AG-5000B) using a 9.5 mm ⁇ punch (tableting pressure: 7.5 KN/punch, weight per tablet: 398.3 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 40 0 C for 16 hr.
  • composition of preparation (398.3 mg) compound A 50 mg lactose 254.6 mg crystalline cellulose ' 37.5 mg hydroxypropylcellulose 14.1 mg monosodium fumarate 23.4 mg low-substituted hydroxypropylcellulose 18.7 mg total 398.3 mg
  • Reference Example 2 In a fluid bed granulator (Lab-1, POWREX CORPORATION), compound A (42.68 g) , lactose (217.32 g) and crystalline cellulose (32 g) were uniformly mixed, granulated by spraying an aqueous solution of hydroxypropylcellulose (12 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules. The sieved granules (15.2 g) and low- substituted hydroxypropylcellulose (0.8 g) were mixed in a glass bottle to give mixed granules.
  • Crystalline cellulose (324 g) , crospovidone (216 g) , magnesium stearate (32.4 g) and the sieved granules (2668 g) were mixed in a tumbler mixer (TM-15, Showa Chemical Machinery) to give mixed granules .
  • the mixed granules were tableted by a rotary tableting machine (VEL50306SS2MZ, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14.8 mm, minor diameter 8 mm) (tableting pressure: 8 KN/punch, weight per tablet: 540 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 40°C for 15 hr.
  • composition of preparation (540 mg) chlorthalidone 25 mg compound A 85.36 mg mannitol 291.04 mg crystalline cellulose 27 mg hydroxypropylcellulose 16.2 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg total 540 mg
  • the mixed granules were tableted by a rotary tableting machine (VEL50306SS2MZ, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14.8 mm, minor diameter 8 mm) (tableting pressure: 8
  • composition of preparation (540 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 179.24 mg crystalline cellulose 18 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg total 540 mg
  • HPLC conditions detector ultraviolet absorption photometer, measurement wavelength: 240 nm column: YMC-Pack ProC18, 5 ⁇ m, inner diameter: 4.6 mm, length: 150 mm column temperature: 25°C mobile phase
  • A 0.05 mol/L phosphate buffer (pH 3.0) /acetonitrile mixed solution (9:1)
  • flow 1 mL/min gradient program (linear) time (min) mobile phase (A) (%) mobile phase (B) (%) 0 (injecting) 100 0
  • Table 1 As shown in Table 1, by separately granulating each compound, the decomposition of compound A was suppressed. [0119] Table 1 preparation increase (%) in amount of decomposed products tablet of Example 1 2. 53 tablet of Example 13 6. 52
  • Example 14 The dried core tablets obtained in Example 14 and Reference Example 3 were stored in a closed glass bottle with a desiccant at 40 0 C for 1 month. An increase in the amount of decomposed products was measured by the following method.
  • HPLC conditions detector ultraviolet absorption spectrophotometer, measurement wavelength: 240 nm column: YMC-Pack ProC18, 5 ⁇ m, inner diameter: 4.6 mm, length: 150 mm column temperature: 25°C mobile phase
  • A 0.05 mol/L phosphate buffer (pH 4.0) /acetonitrile/tetrahydrofuran mixed solution (40:7:3)
  • B acetonitrile/O.05 mol/L phosphate buffer (pH 4.0) /tetrahydrofuran mixed solution (49:30:21) flow: 1 mL/min gradient program (linear)
  • Example 14 and Example 15 were stored in a closed glass bottle with a desiccant at 40 0 C for 1 month.
  • An increase in the amount of decomposed products was measured in the same manner as in Experimental Example 3.
  • Table 3 As show in Table 3, by separately granulating each compound, the decomposition of compound A was suppressed.
  • the solid preparation of the present invention is useful for the prophylaxis or treatment of circulatory diseases such as hypertension, cardiac failure, diabetic nephropathy, arteriosclerosis and the like.
  • the solid preparation of the present invention comprising the aforementioned compound represented by the formula (I) , a pH control agent and a diuretic shows superior safety and superior dissolution property of the compound represented by the formula (I) and the diuretic.

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Abstract

The present invention relates to a solid preparation containing a compound represented by the formula (I) wherein each symbol is as defined in the specification, or a salt thereof, a pH control agent and a diuretic, which is superior in the stability and dissolution property of the compound represented by the formula (I) and the diuretic.

Description

DESCRIPTION SOLID PHAERMACEUTICAL COMPOSITION
TECHNICAL FIELD OF THE INVENTION [0001] The present invention relates to a solid preparation comprising a compound represented by the formula (I) to be shown below, a pH control agent and a diuretic, which is superior in the stability and dissolution property of the compound (I) and the diuretic. [0002]
(Background of the Invention)
It is important that pharmaceutical products be effective and safe. Even when a pharmaceutical product is effective and safe immediately after production, if the drug is easily decomposed or denatured during storage and distribution of the pharmaceutical product, it is not considered to be effective and safe as a pharmaceutical product. Therefore, the stability of the drug is extremely important for pharmaceutical products. [0003] To secure effectiveness and safety of a pharmaceutical product, not only the effectiveness and safety of the active ingredient itself are important but also the properties of the pharmaceutical preparation such as the drug dissolution property and the like in the body are extremely important. For example, when the dissolution of the drug from the pharmaceutical preparation is too late, the blood concentration of the drug does not reach an effective level, and the expected efficacy may not be sufficiently exhibited. On the other hand, when the dissolution of the drug from the preparation is too fast, the blood concentration of the drug increases sharply, causing a high risk of side effects.
In other words, pharmaceutical products are required to ensure, in addition to effectiveness and safety, the stability of the drug and a certain level of the drug dissolution property. The dissolution property of a drug is known to correlate with the solubility thereof. In general, lower solubility of a drug is known to cause slower dissolution property of the drug. [0004] A benzimidazole derivative having a strong angiotensin II receptor antagonistic activity, which is represented by the formula (I)
wherein R1 is a monocyclic nitrogen-containing heterocyclic group having a deprotonizable hydrogen atom, R2 is an esterified carboxyl group and R3 is an optionally substituted lower alkyl, or a salt thereof (hereinafter sometimes to be referred to as compound (I) ) , particularly (5-methyl-2-oxo- 1, 3-dioxol-4-yl) methyl 2-ethoxy-l-{ [2' - (5-oxo-4, 5-dihydro- 1,2, 4-oxadiazol-3-yl) biphenyl-4-yl]methyl } -lH-benzimidazole-7- carboxylate salt (patent document 1) , is considered to be a promising therapeutic drug for hypertension and the like. However, the properties of a pharmaceutical preparation containing compound (I) need to be controlled to stabilize compound (I) because compound (I) is unstable in the neutral pH range, at which the pharmaceutical preparation is generally produced. Nevertheless, the solubility of compound (I) is low at the pH range where compound (I) is stable. In addition, a combination drug product composed of compound (I) and other active ingredient such as diuretic and the like cannot be easily formulated into a preparation superior in stability and dissolution property since the chemical properties are different. [0005] As a combination drug product, a combination of a compound having an angiotensin II antagonistic activity and a compound having a diuretic action (patent document 2), and an internal solid preparation containing acetaminophen granules obtained by a separating granulation method to suppress the unpleasant taste and prevent discoloration of acetaminophen
(patent document 3) are known. However, a combination drug product of compound (I) and a diuretic, which simultaneously affords drug stability and solubility, namely, dissolution property, has not been known. CITATION LIST
PATENT LITERATURE patent document 1: WO2005/080384 patent document 2: US-B-5721263 patent document 3: JP-A-2001-294524 SUMMARY OF THE INVENTION
PROBLEMS TO BE SOLVED BY THE INVENTION
[0006]
A preparation containing compound (I) and a diuretic is effective for the prophylaxis or treatment of circulatory diseases such as hypertension, cardiac failure, diabetic nephropathy, arteriosclerosis and the like, and has extremely high clinical usefulness.
The problem of the present invention is to provide a solid preparation superior in the stability of compound (I) and a diuretic as well as the dissolution property thereof.
MEANS OF SOLVING THE PROBLEMS
[0007]
The present inventors have conducted intensive studies in an attempt to simultaneously achieve the stability of compound (I) in a preparation and dissolution property thereof from the preparation, and found that the objects can be unexpectedly accomplished by the co-presence of a pH control agent and compound (I), and further, by adjusting, with a pH control agent, the pH range of a solid preparation thereof to a pH range in which the solubility of compound (I) becomes low. In addition, they have found that a diuretic and compound (I) containing a pH control agent can be further stabilized by separately granulating them, whereby a preparation more superior in the dissolution property of compound (I) as compared to general granulation preparations can be obtained, which resulted in the completion of the present invention. [0008]
Accordingly, the present invention relates to: [1] a solid preparation comprising a compound represented by the formula (I):
wherein R1 is a monocyclic nitrogen-containing heterocyclic group having a deprotonizable hydrogen atom, R2 is an esterified carboxyl group and R3 is an optionally substituted lower alkyl, or a salt thereof, a pH control agent and a diuretic,
[2] the solid preparation of [1] , wherein the compound represented by the formula (I) or a salt thereof is (5-methyl- 2-oxo-l,3-dioxol-4-yl)methyl 2-ethoxy-l-{ [2' - (5-oxo-4 , 5- dihydro-1, 2, 4-oxadiazol-3-yl) biphenyl-4-yl] methyl} -IH- benzimidazole-7-carboxylate potassium salt,
[3] the solid preparation of [1] or [2], wherein the diuretic is chlorthalidone or hydrochlorothiazide, [4] the solid preparation of [1], wherein the salt of the compound represented by the formula (I) is (5-methyl-2-oxo- 1, 3-dioxol-4-yl) methyl 2-ethoxy-l-{ [2' - (5-oxo-4, 5-dihydro- 1,2, 4-oxadiazol-3-yl) biphenyl-4-yl] methyl }-lH-benzimidazole-7- carboxylate potassium salt, and the diuretic is chlorthalidone, [5] the solid preparation of [1], wherein the pH control agent has pH 2 to 5, [6] the solid preparation of [1], wherein the pH control agent is an acidic substance selected from the group consisting of tartaric acid, citric acid, lactic acid, fumaric acid, succinic acid, phosphoric acid, malic acid, ascorbic acid, acetic acid and acidic amino acid, or a salt thereof, or a solvate thereof,
[7] the solid preparation of [1], wherein the pH control agent is monosodium fumarate, or a combination of fumaric acid and sodium ion donor, [8] a solid preparation comprising a first part comprising a compound represented by the formula (I):
wherein R1 is a monocyclic nitrogen-containing heterocyclic group having a deprotonizable hydrogen atom, R2 is an esterified carboxyl group and R3 is an optionally substituted lower alkyl, or a salt thereof and a pH control agent, and a second part comprising a diuretic, which is obtained by granulating separately from the first part, [9] the solid preparation of [1], wherein the compound represented by the formula (I), or a salt thereof and the pH control agent are contained in a first part and the diuretic is contained in a second part, which is a multi-layer tablet comprising a first layer comprised of the first part and a second layer comprised of the second part, [10] the solid preparation of [1], wherein the pH control agent is in a proportion of 0.01-20 wt% of the preparation, [11] a method of stabilizing a compound represented by the formula (I) or a salt thereof and a diuretic in a solid preparation, which comprises adding a pH control agent to the solid preparation, [12] a method of improving dissolution property of a compound represented by the formula (I) or a salt thereof from a solid preparation comprising the compound or the salt thereof and a diuretic, which comprises adding a pH control agent to the solid preparation; and the like.
EFFECT OF THE INVENTION
[0009]
The solid preparation of the present invention comprising compound (I) , a pH control agent and a diuretic can provide a preparation superior in the stability and dissolution property of compound (I) and the diuretic.
BRIEF DESCRIPTION OF THE DRAWINGS
[0010] Fig. 1 shows dissolution profiles of the tablets obtained in Example 14 and Reference Example 3.
Fig. 2 shows dissolution profiles of the tablets obtained in Example 15 and Reference Example 4.
DESCRIPTION OF EMBODIMENTS [0011]
The solid preparation of the present invention is explained in detail in the following.
The solid preparation of the present invention contains compound (I) , a pH control agent and a diuretic (also referred to as the solid preparation of the present invention) . The solid preparation of the present invention is superior in the stability of compound (I) , and also superior in the dissolution property of the compound (I) . It is also superior in the stability of the diuretic. [0012]
In the aforementioned formula (I), R1 is a monocyclic nitrogen-containing heterocyclic group having a hydrogen atom that can be deprotonized, such as a tetrazolyl group or a group represented by the formula wherein i is -O- or -S-, j is >C=0, >C=S or >S(0)m wherein m is 0, 1 or 2 (e.g., 4, 5-dihydro-5-oxo-l, 2, 4-oxadiazol-3-yl group, etc.) and the like are preferable. A 4, 5-dihydro-5-oxo-l,2, 4-oxadiazol-3-yl group includes three tautomers (a', b' and c' ) represented by the formulas:
^
a1 b1 c1 and 4, 5-dihydro-5-oxo-l, 2, 4-oxadiazol-3-yl group includes all of the above-mentioned a' , b' and c' . [0013]
In the aforementioned formula (I), R2 is an esterified carboxyl group and, for example, preferably a carboxyl group esterified by lower (Ci_4)alkyl optionally substituted by a substituent selected from a hydroxyl group, an amino group, a halogen atom, lower (C2-6) alkanoyloxy (e.g., acetyloxy, pivaloyloxy, etc.), lower (C4-.-?) cycloalkanoyloxy, (lower (Ci- s) alkoxy) carbonyloxy (e.g., methoxycarbonyloxy, ethoxycarbonyloxy, etc.), (lower (C3-7) cycloalkoxy) carbonyloxy (e.g., cyclohexyloxycarbonyloxy, etc.), lower (C1-4) alkoxy and 5-methyl-2-oxo-l, 3-dioxolen-4-yl (e.g., (5-methyl-2-oxo-l, 3- dioxolen-4-yl)methoxycarbonyl group, 1-
(cyclohexyloxycarbonyloxy) ethoxycarbonyl group and the like). [0014]
In the aforementioned formula (I), R3 is an optionally substituted lower alkyl, and preferably a lower (d-5)alkyl optionally substituted by a substituent selected from a hydroxyl group, an amino group, a halogen atom and a lower (C1-4) alkoxy group (preferably lower (C2-3) alkyl; particularly preferably ethyl) . [0015] The salt of a compound represented by the formula (I) is, for example, a pharmaceutically acceptable salt. Examples of the salt of a compound represented by the formula (I) include a salt with an inorganic base, a salt with an organic base, a salt with an inorganic acid, a salt with an organic acid, a salt with a basic or acidic amino acid and the like. Preferable examples of the salt with an inorganic base include alkali metal salt such as sodium salt, potassium salt and the like; alkaline earth metal salt such as calcium salt, magnesium salt and the like; aluminum salt, ammonium salt and the like. Preferable examples of the salt with an organic base include salts with trimethylamine, triethylamine, pyridine, picoline, ethanolamine, diethanolamine, triethanolamine, dicyclohexylamine, N, N' -dibenzylethylenediamine and the like. Preferable examples of the salt with an inorganic acid include salts with hydrochloric acid, hydrobromic acid, nitric acid, sulfuric acid, phosphoric acid and the like. Preferable examples of the salt with an organic acid include salts with formic acid, acetic acid, trifluoroacetic acid, fumaric acid, oxalic acid, tartaric acid, maleic acid, citric acid, succinic acid, malic acid, methanesulfonic acid, benzenesulfonic acid, p-toluenesulfonic acid and the like. Preferable examples of the salt with a basic amino acid include salts with arginine, lysine, ornithine and the like, and preferable examples of salts with acidic amino acid include salts with aspartic acid, glutamic acid and the like. [0016]
As a compound represented by the formula (I) or a salt thereof, a salt of (5-methyl-2-oxo-l, 3-dioxol-4-yl) methyl 2- ethoxy-l-{ [2' - (5-oxo-4, 5-dihydro-l, 2, 4-oxadiazol-3- yl) biphenyl-4-yl]methyl}-lH-benzimidazole-7-carboxylate is preferable, and (5-methyl-2-oxo-l, 3-dioxol-4-yl)methyl 2- ethoxy-l-{ [2' - (5-oxo-4, 5-dihydro-l, 2, 4-oxadiazol-3- yl ) biphenyl-4-yl] methyl } -lH-benzimidazole-7-carboxylate potassium salt is particularly preferable. The salt of a compound represented by the formula (I)' may¬ be hydrate or non-hydrate.
Compound (I) may be a solvate including hydrate or a non- solvate . [0017]
Compound (I) is preferably in the form of a crystal, and preferably has a melting point of 100 - 2500C, particularly 120 - 2000C, especially 130 - 1800C. [0018] Compound (I) is contained in the solid preparation of the present invention in a proportion of 0.1 - 60 wt%, preferably 1 - 40 wt%, more preferably 5 - 30 wt%. [0019]
The pH control agent to be used in the present invention may be any as long as it simultaneously achieves stability of the preparation of compound (I) and dissolution property of compound (I) from the preparation and is applicable to a pharmaceutical product. In addition, plural pH control agents may be used in combination. The pH control agent to be used in the present invention preferably has a pH of about 2 to about 5, preferably about 3 to about 5, more preferably about 3 to about 4. For example, an acidic substance such as tartaric acid, citric acid, lactic acid, fumaric acid, phosphoric acid, malic acid, succinic acid, ascorbic acid, acetic acid, acidic amino acid (e.g., glutamic acid, aspartic acid) and the like, an inorganic salt (e.g., alkali metal salt, alkaline earth metal salt, ammonium salt and the like) of these acidic substances, a salt of such acidic substance with an organic base (e.g., basic amino acid such as lysine, arginine and the like, meglumine and the like), a solvate (e.g., hydrate) thereof and the like are used. The pH control agent simultaneously achieves stability of a diuretic and dissolution property of the diuretic from the preparation.
Here, the pH of the pH control agent is measured under the following conditions. To be specific, it is the pH of a solution or suspension obtained by dissolving or suspending a pH control agent in water at 25°C at a concentration of 1 w/v% . [0020]
As the pH control agent to be used in the present invention, an acidic substance and a basic substance are combined, and the obtained pH control agent may be adjusted such that the pH of the solution or suspension is about 2 to about 5, preferably about 3 to about 5, more preferably about 3 to about 4, when the combined pH control agent is dissolved or suspended in water at 25°C at a concentration of 1 w/v% . Examples of the acidic substance to be used in combination include, in addition to the acidic substances having a pH of about 2 to about 5 mentioned above and salts thereof, strong acids such as hydrochloric acid, sulfuric acid, phosphoric acid and like. Examples of the basic substance to be used in combination include inorganic bases (e.g., sodium hydroxide, potassium hydroxide, sodium carbonate, sodium hydrogen carbonate, magnesium carbonate, calcium carbonate, magnesium oxide, ammonia, synthetic hydrotalcite) , organic bases (e.g., basic amino acid such as lysine, arginine, etc., meglumine, and the like) and the like.
The pH control agent to be used in the present invention preferably affords a solution having a buffering capacity at pH 2 to 5, such as sodium dihydrogen phosphate, monosodium fumarate, a combination of fumaric acid and sodium ion donor and the like.
The pH control agent to be used in the present invention is preferably monosodium fumarate or a combination of fumaric acid and sodium ion donor. In addition, fumaric acid and sodium hydroxide may be used in combination. [0021]
In the solid preparation of the present invention, the pH control agent is contained in a proportion of 0.01 - 20 wt%, preferably 0.05 - 10 wt%, more preferably 0.1 - 5 wt%, of the solid preparation. [ 0022 ]
Examples of the diuretic in the present invention include xanthine derivatives (e.g., theobromine sodium salicylate, theobromine calcium salicylate etc.), thiazide preparations (e.g., ethiazide, cyclopenthiazide, trichloromethyazide, hydrochlorothiazide, hydroflumethiazide, benzylhydrochlorothiazide, penflutizide, polythiazide, methyclothiazide etc.), antialdosterone preparations (e.g., spironolactone, triamterene etc.), carbonic anhydrase inhibitors (e.g., acetazolamide etc.), chlorobenzenesulfonamide agents (e.g., chlorthalidone, mefruside, indapamide etc.), azosemide, isosorbide, ethacrynic acid, piretanide, bumetanide, furosemide and the like. The diuretic in the present invention also includes salts of the compounds recited as the above-mentioned diuretic. As the diuretic in the present invention, a chlorobenzenesulfonamide agent, a thiazide preparation and the like are preferable, and chlorthalidone, hydrochlorothiazide and the like are more preferable. Especially, chlorthalidone is preferable. [0023]
In the present invention, the diuretic is contained in the solid preparation in a proportion of generally, 0.1 - 60 wt% (appropriately adjusted so that the total of compound (I) and pH control agent will not exceed 100%), preferably 0.5 - 40 wt%, more preferably 1 - 30 wt%. Specifically, chlorthalidone (converted into a free form) is contained in a proportion of generally 0.1 - 60 wt%, preferably 0.5 - 40 wt%, more preferably 1 - 30 wt%. Hydrochlorothiazide (converted into a free form) is contained in a proportion of generally 0.1 - 60 wt%, preferably 0.5 - 40 wt%, more preferably 1 - 30 wt%. [0024]
A preferable form of the solid preparation of the present invention is a preparation wherein compound (I) is (5-methyl- 2-oxo-l, 3-dioxol-4-yl) methyl 2-ethoxy-l-{ [2' - (5-oxo-4, 5- dihydro-1, 2, 4-oxadiazol-3-yl) biphβnyl-4-yl]methyl}-lH- benzimidazole-7-carboxylate potassium salt and the diuretic is chlorthalidone . [0025]
Examples of the solid preparation of the present invention include a solid preparation suitable for oral administration such as tablets, granules, fine granules, capsules, pills and the like. Therefore, the embodiments of the solid preparation of the present invention include the following preparations. (1) A solid preparation obtained by mixing and granulating compound (I) , a pH control agent and a diuretic (single granulation preparation) . (2) A solid preparation containing a first part containing compound (I) and a pH control agent, and a second part containing a diuretic, which is obtained by separately granulating the first part and the second part (separating granulation preparation - a single layer tablet) . (3) A solid preparation obtained by compression-molding a first part containing compound (I) and a pH control agent, and a second part containing a diuretic independently, which are separately granulated (separating granulation preparation - a multi-layer tablet) , or by coating one part with the other part, which are separately granulated (separating granulation preparation - coated tablet) . [0026]
The solid preparation of the above-mentioned (1) simultaneously achieves dissolution property and stability of compound (I) and a diuretic respectively in and from the preparation thereof by the addition of a pH control agent. In the above-mentioned (2) and (3) , the dissolution property and stability of compound (I) and the diuretic are respectively improved further. [0027] The solid preparation of the above-mentioned (1) can -be produced by a method known per se (e.g., method described in the Japanese Pharmacopoeia 14th Edition, General Rules for Preparations) . For example, compound (I), a pH control agent, a diuretic, additives and the like are mixed, a binder is added to the mixture to give granules, a lubricant and the like are added to the granules and the mixture is tableted into a tablet. Granules and fine granules can also be produced by a method similar to that of the tablet.
In the case of a capsule, the above-mentioned granules and fine granules are filled in a capsule containing gelatin, hydroxypropylmethylcellulose and the like. Alternatively, an active ingredient and a filler are filled in a capsule containing gelatin, hydroxypropylmethylcellulose and the like. [0028]
The solid preparation may contain additives conventionally used in the pharmaceutical field. Examples of the additive include filler, disintegrant, binder, lubricant, colorant, pH control agent, surfactant, stabilizer, acidulant, flavor, glidant and the like. These additives are used in an amount conventionally employed in the pharmaceutical field. [0029]
Examples of the filler include starches such as cornstarch, potato starch, wheat starch, rice starch, partly pregelatinized starch, pregelatinized starch, porous starch and the like; sugar and sugar alcohols such as lactose, fructose, glucose, mannitol (e.g., D-mannitol) , sorbitol (e.g., D-sorbitol) , erythritol (e.g., D-erythritol) , sucrose and the like; anhydrous calcium phosphate, crystalline cellulose, microcrystalline cellulose, glycyrrhiza uralensis, sodium hydrogen carbonate, calcium phosphate, calcium sulfate, calcium carbonate, precipitated calcium carbonate, calcium silicate and the like. [0030] Examples of the disintegrant include amino acid, starch? cornstarch, carboxymethylcellulose, calcium carboxymethylcellulose, sodium carboxymethyl starch, carmellose sodium, carmellose calcium, croscarmellose sodium, crospovidone, low-substituted hydroxypropylcellulose, hydroxypropylstarch, sodium carboxymethyl starch and the like. [0031]
Examples of the binder include crystalline cellulose (e.g., microcrystalline cellulose), hydroxypropylcellulose, hydroxypropylmethylcellulose, polyvinylpyrrolidone, gelatin, starch, gum arabic powder, tragacanth, carboxymethylcellulose, sodium alginate, pullulan, glycerol and the like. [0032]
Preferable examples of the lubricant include magnesium stearate, stearic acid, calcium stearate, talc (purified talc) , sucrose esters of fatty acids, stearyl fumarate monosodium salt and the like. [0033]
Examples of the colorant include food colors such as Food Color Yellow No. 5, Food Color Red No. 2, Food Color Blue No. 2 and the like, food lake colors, diiron trioxide and the like. [0034]
Examples of the surfactant include sodium lauryl sulfate, polysorbate 80, polyoxyethylene (160) polyoxypropylene (30) glycol and the like.
Examples of the stabilizer include tocopherol, tetrasodium edetate, nicotinic acid amide, cyclodextrins and the like. [0035] Examples of the acidulant include ascorbic acid, citric acid, tartaric acid, malic acid and the like.
Examples of the flavor include menthol, peppermint oil, lemon oil, vanillin and the like.
Examples of the glidant include light anhydrous silicic acid, hydrated silicon dioxide and the like. The above-mentioned additives may be a mixture of two ■■ or more kinds at an appropriate ratio. [0036]
The solid preparation of the above-mentioned (2) contains a first part and a second part, which are separately granulated, and can be produced by a method known per se.
In the solid preparation of the above-mentioned (2), the first part in the present invention is a part (composition) containing compound (I) and a pH control agent. [0037]
The amount of the pH control agent to be used in the present invention is preferably 0.01 - 20 parts by weight, preferably 0.05 - 10 parts by weight, more preferably 0.1 - 5 parts by weight, per 100 parts by weight of the above- mentioned first part. [0038]
The weight ratio of compound (I) to a pH control agent (compound (I): pH control agent) is preferably 1 - 30:1, more preferably 5 - 25:1, more preferably 10 - 20:1. [0039]
The above-mentioned first part is not limited as long as it has a shape and a size that afford a solid preparation together with the below-mentioned second part. [0040] The above-mentioned first part may further contain additives conventionally used in the pharmaceutical field. As the additives, those similar to the aforementioned additives can be used.
The above-mentioned first part can be produced by mixing compound (I), a pH control agent and, where necessary, the above-mentioned additives and granulating the mixture according to a method known per se. [0041]
The above-mentioned first part preferably contains compound (I) (preferably (5-methyl-2-oxo-l, 3-dioxol-4- yl) methyl 2-ethoxy-l-{ [2' - (5-oxo-4, 5-dihydro-l, 2, 4-oxadiazol-
3-yl) biphenyl-4-yl] methyl } -lH-benzimidazole-7-carboxylate potassium salt) ; a pH control agent (preferably fumaric acid and sodium hydroxide) ; a filler (preferably mannitol and crystalline cellulose) ; and a binder (preferably hydroxypropylcellulose) .
[0042]
The second part in the present invention is a part
(composition) containing a diuretic. The above-mentioned second part is not limited as long as it has a shape and a size that afford a solid preparation together with the above-mentioned first part .
[0043]
The above-mentioned second part may further contain additives conventionally used in the pharmaceutical field. As the additives, those similar to the aforementioned additives can be used.
Specifically, it contains a diuretic (preferably chlorthalidone) ; a filler (preferably mannitol and crystalline cellulose) ; and a binder (preferably hydroxypropylcellulose) .
[0044]
The above-mentioned second part can be produced by mixing a diuretic and, where necessary, the above-mentioned additives and granulating the mixture according to a method known per se. The amount of the diuretic is preferably 0.1 - 60 parts by weight, more preferably 0.5 - 40 parts by weight, more preferably 1 - 30 parts by weight, per 100 parts by weight of the above-mentioned second part.
[0045] The weight ratio of the second part to the first part in the solid preparation of the present invention (second part: first part) is preferably 0.1 - 10:1, more preferably 0.3
- 5:1, more preferably, 0.5 - 3:1.
A single layer tablet produced by mixing a first part and a second part, which are separately granulated, and further, additives conventionally used in the pharmaceutical field, and then compressing the mixture is also encompassed in the solid preparation of the present invention. A capsule produced by- filling the above-mentioned single layer tablet in a capsule (e.g., hydroxypropylmethylcellulose capsule) is also encompassed in the solid preparation of the present invention.
A capsule produced by directly filling the first part and the second part, which are separately granulated, or together with the above-mentioned additives, in a capsule (e.g., hydroxypropylmethylcellulose capsule) is also encompassed in the solid preparation of the present invention. [0046]
In the solid preparation of the above-mentioned (3) , the first part and the second part are separately granulated, and the preparation can be produced by compressing independently these parts, or coating one part with the other part. [0047]
Specific examples of the solid preparation of the above- mentioned (3) include [1] coated tablet (A) containing an inner core of the first part and an outer layer of the second part; [2] coated tablet (B) containing an inner core of the second part and an outer layer of the first part; [3] a multilayer tablet containing a first layer of the first part and a second layer of the second part. [0048]
The inner core of the first part can be produced by, for example, granulating compound (I) , a pH control agent and, where necessary, additives. After granulation, where necessary, an operation of drying, sieving, compression and the like may be applied. [0049]
The outer layer of the second part can be produced, for example, by granulating a diuretic (e.g., chlorthalidone or a salt thereof) with additives, as necessary. The coating can be performed, for example, by compression, coating and the like. The additive is preferably a binder and the like.
[0050]
For production of coated tablet (A) , an inactive intermediate layer may be inserted between an inner core and an outer layer to prevent a direct contact. The intermediate layer contains, for example, the following coating base and additives for coating. The intermediate layer preferably contains a water-soluble film coating base and a glidant. [0051]
The above-mentioned coated tablet (B) can be produced in the same manner as in coated tablet (A) except that the second part is used as an inner core and first part is used as an outer layer. [0052]
The multi-layer tablet of the present invention comprises a first part containing a compound represented by the formula
(I) or a salt thereof and a pH control agent and a second part containing a diuretic, wherein a first layer is comprised of the first part and a second layer is comprised of the second part.
[0053]
The multi-layer tablet of the present invention is not particularly limited as long as it is a preparation wherein at least the first layer comprised of the first part and the second layer comprised of the second part are integrally formed.
[0054]
In addition, the multi-layer tablet in the present invention may have an inactive intermediate layer between the first layer and the second layer.
[0055]
When the multi-layer tablet in the present invention has such intermediate layer, the adverse influences (decreased preservation stability such as time-course decomposition of active ingredients, lowered effectiveness and the like, decreased dissolution stability such as time-course changes in dissolution pattern of active ingredients and the like, and so on) produced by interaction between the active ingredients can be more effectively suppressed. [0056]
The multi-layer tablet can be produced, for example, by the following production steps.
Compound (I) and a pH control agent are mixed with additives as necessary, and the obtained mixture is granulated to give the first part. After granulation, operations such as drying, sieving and the like may be performed where necessary. Thereafter, additives are mixed where necessary to give the first layer. Then, a diuretic is granulated with additives as necessary, and the obtained second part is mixed with additives as necessary to give the second layer, which is put on the above-mentioned first layer in layers and compressed (preferably tableted) . To prevent a direct contact of respective layers, an inactive intermediate layer may be inserted between the respective layers. The intermediate layer contains, for example, the above-mentioned filler, disintegrant, binder, lubricant, colorant and the like. [0057]
A capsule produced by filling the above-mentioned coated tablet (A) or (B) or multi-layer tablet in a capsule (e.g., hydroxypropylmethylcellulose capsule) is also encompassed in the solid preparation of the present invention. [0058]
In addition, a film coating preparation produced by coating the above-mentioned solid preparation (1) - (3) with a film of the following coating base and additives for coating is also encompassed in the solid preparation of the present invention. [ 0059]
Preferable examples of the coating base include a sugar coating base, a water-soluble film coating base, an enteric film coating base, a sustained-release film coating base and the like. [0060]
As the sugar coating base, sucrose is used. Moreover, one or more kinds selected from talc, precipitated calcium carbonate, gelatin, gum arabic, pullulan, carnauba wax and the like may also be used concurrently. [0061]
Examples of the water-soluble film coating base include cellulose polymers such as hydroxypropylcellulose [e.g., grade: L, SL, SL-T, SSL (trade name); Nippon Soda Co., Ltd.], hydroxypropylmethylcellulose [e.g., TC-5 (grade: MW, E, EW, R, RW) (trade name); Shin-Etsu Chemical Co., Ltd.], hydroxyethylcellulose, methylhydroxyethylcellulose and the like; synthetic polymers such as polyvinyl acetaldiethylaminoacetate, aminoalkylmethacrylate copolymer E [Eudragit E (trade name) ] , polyvinylpyrrolidone and the like; polysaccharides such as pullulan and the like, and so on. [0062]
Examples of the enteric film coating base include cellulose polymers such as hydroxypropylmethylcellulose phthalate, hydroxypropylmethylcellulose acetatesuccinate, carboxymethylethylcellulose, cellulose acetate phthalate and the like; acrylic acid polymers such as methacrylic acid copolymer L [Eudragit L (trade name) ] , methacrylic acid copolymer LD [Eudragit L-30D55 (trade name) ] , methacrylic acid copolymer S [Eudragit S (trade name) ] and the like; naturally occurring substance such as shellac and the like, and so on. [0063]
Examples of the sustained-release film coating base include cellulose polymers such as ethylcellulose and the like; acrylic acid polymers such as aminoalkylmethacrylate copolymer RS [Eudragit RS (trade name) ] , ethyl acrylate-methyl - methacrylate copolymer suspension [Eudragit NE (trade name) ] and the like, and so on.
[0064] Preferable examples of the coating additives include light protecting agents such as titanium oxide and the like, glidants such as talc and the like, colorants such as red ferric oxide, yellow ferric oxide and the like; plasticizers such as polyethylene glycol [e.g., macrogol 6000 (trade name)], triethyl citrate, castor oil, polysorbate and the like; organic acids such as citric acid, tartaric acid, malic acid, ascorbic acid and the like; and so on.
[0065]
Moreover, the solid preparation of the present invention may have a distinguishable embossing or printed letters, or a scored line for division.
[0066]
The solid preparation of the present invention is preferably film-coated from the aspects of easy administration, mechanical strength and the like.
In the aforementioned production steps, operations such as mixing, compression, coating and the like are performed according to the methods conventionally used in the pharmaceutical technological field. [0067]
The mixing is performed, for example, using a blending machine such as a V-type mixer, a tumbler mixer and the like; and a granulator such as a high speed mixer granulator, a fluid bed granulator, an extrusion-granulator, a roller compactor and the like.
[0068]
The compression is performed, for example, using a single stroke tableting machine, a rotary tableting machine and the like. When compression is performed using a single stroke tableting machine, a rotary tableting machine and the like, a tableting pressure of generally 1 - 20 kN/cm2 (preferably 5 - 15 kN/cm2) is preferably employed. In addition, a taper cutting die is preferably used for preventing capping. [0069]
The coating is performed, for example, using a film coating apparatus and the like. [0070]
The solid preparation of the present invention can be used safely as a medicine for mammals (e.g., human, dog, rabbit, rat, mouse and the like) .
While the dose of compound (I) to patients is determined in consideration of age, body weight, general health condition, sex, diet, administration time, clearance rate, combination of drugs and the like, as well as the severity of the disease for which the patient is undergoing treatments, the daily dose is about 0.05 - 500 mg, preferably 0.1 - 100 mg.
While the dose of a diuretic to patients is determined in consideration of age, body weight, general health condition, sex, diet, administration time, clearance rate, combination of drugs and the like, as well as the severity of the disease for which the patient is undergoing treatments, the daily dose is, for example, about 12.5 - 100 mg, preferably 15 - 50 mg, of chlorthalidone (converted into free form) . In the case of hydrochlorothiazide (converted into free form) , the daily dose is about 12.5 - 100 mg, preferably 15 - 50 mg. [0071]
Since compound (I) has a strong angiotensin II antagonistic activity, the pharmaceutical composition of the present invention is useful as a prophylactic or therapeutic drug for diseases developed by (or diseases whose onset is promoted by) contraction or growth of blood vessel or an organ disorder expressed via angiotensin II receptor, due to the presence of angiotensin II, or a factor induced by the presence of angiotensin II, in mammals (e.g., human, monkey, cat, swine, horse, bovine, mouse, rat, guinea pig, dog, rabbit and the like) .
By combination of compound (I) and a diuretic, the solid preparation of the present invention is useful as a prophylactic or therapeutic drug for the above-mentioned diseases, can reduce the doses of compound (I) and a diuretic as compared to independent use thereof and can suppress expression of side effects. [0072] The present invention provides a method of stabilizing a compound represented by the formula (I) or a salt thereof and a diuretic in a solid preparation containing a compound represented by the formula (I) or a salt thereof, and a diuretic, which includes adding a pH control agent. According to the stabilizing method of the present invention, compound (I) and a diuretic in a solid preparation is significantly stabilized. In addition, the present invention provides a method of improving dissolution of a compound represented by the formula (I) or a salt thereof from a solid preparation containing the compound or a salt thereof, and a diuretic, which includes adding a pH control agent. According to the improving method of dissolution property in the present invention, the dissolution property of compound (I) and a diuretic from a solid preparation is significantly improved. EXAMPLES [0073]
The present invention is explained in more detail in the following by referring to Examples and Experimental Examples, which are not to be construed as limitative. In the formulations described in the Example, the components (additives) other than the active ingredient may be those recited in the Japanese Pharmacopoeia, the Japanese Pharmacopoeia Japanese Pharmaceutical Codex or Japanese Pharmaceutical Excipients and the like. [0074] Example 1
(1) In a fluid bed granulator (FD-5S, POWREX CORPORATION), (5- methyl-2-oxo-l, 3-dioxol-4-yl) methyl 2-ethoxy-l-{ [2'-(5-oxo-
4, 5-dihydro-l, 2, 4-oxadiazol-3-yl) biphenyl-4-yl] methyl} -IH- benzimidazole-7-carboxylate potassium salt (hereinafter to be referred to as compound A) (1067 g) and mannitol (1968 g) were uniformly mixed, granulated by spraying an aqueous solution of hydroxypropylcellulose (112.5 g) , fumaric acid (46.5 g) and sodium hydroxide (16 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules A.
(2) In a fluid bed granulator (Lab-1, POWREX CORPORATION), chlorthalidone (300 g) , and mannitol (402 g) were uniformly mixed, granulated by spraying an aqueous solution of hydroxypropylcellulose (27 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules B.
(3) Croscarmellose sodium (24.68 g) , crystalline cellulose (30.86 g) , magnesium stearate (3.08 g) , the sieved granules A (128.4 g) and the sieved granules B (121.5 g) were mixed in a bag to give mixed granules.
(4) The mixed granules were tableted by a rotary tableting machine (AQUARIUS, Kikusui Seisakusho, Ltd.) using a 7 mmφ punch (tableting pressure: 4 KN/punch, weight per tablet: 154.26 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 400C for 16 hr.
[0075] composition of preparation (154.26 mg) compound A 21.34 mg mannitol 39.36 mg hydroxypropylcellulose 2.25 mg fumaric acid 0.93 mg sodium hydroxide 0.32 mg chlorthalidone 25 mg mannitol 33.5 mg hydroxypropylcellulose 2.25 mg croscarmellose sodium 12.34 mg crystalline cellulose 15.43 mg magnesium stearate 1.54 mg total 154.26 mg
[0076] Example 2
(1) In a fluid bed granulator (Lab-1, POWREX CORPORATION), compound A (256.1 g) and mannitol (429.8 g) were uniformly- mixed, granulated by spraying an aqueous solution of hydroxypropylcellulose (27 g) , fumaric acid (12 g) and sodium hydroxide (4.14 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules A. Croscarmellose sodium (24 g) , crystalline cellulose (30 g) and magnesium stearate (3 g) and the sieved granules A (85.36 g) were mixed in a bag to give mixed granules A.
(2) Crystalline cellulose (granules) was fed into a rotating fluid bed granulator (SPIR-A-FLOW, Freund Corporation) , and a dispersion of chlorthalidone (105 g) , crystalline cellulose (6.3 g) , low-substituted hydroxypropylcellulose (16.8 mg) hydroxypropylmethylcellulose (16.8 g) was sprayed and layered on the crystalline cellulose granules, and dried therein to give granules. The obtained granules were passed through a sieve to give sieved granules B (150 - 500 μm) .
(3) The mixed granules A (3 g) and the sieved granules B (0.525 g) were mixed in a glass bottle to give mixed granules. The obtained mixed granules were tableted by Autograph (SHIMADZU Corporation, AG-5000B) using a 9.5 mmφ punch
(tableting pressure: 7 KN/punch, weight per tablet: 352.5 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 400C for 16 hr. [0077] composition of preparation (352.5 mg) compound A 85.36 mg mannitol 143.26 mg hydroxypropylcellulose 9 mg fumaric acid 4 mg sodium hydroxide 1.38 mg chlorthalidone 25 mg crystalline cellulose (granules) 18 mg crystalline cellulose 1.5 mg low-substituted hydroxypropylcellulose 4 mg hydroxypropylmethylcellulose 4 mg croscarmellose sodium 24 mg crystalline cellulose 30 mg magnesium stearate 3 mg total 352.5 mg
[0078]
Example 3
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator (WSG-60, POWREX CORPORATION), chlorthalidone (5375 g) , mannitol (53450 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION) , compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules B.
(3) Crystalline cellulose (9720 g) , crospovidone (5670 g) , magnesium stearate (972 g) , the milled granules A (54430 g) and the milled granules B (26410 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules .
(4) The mixed granules were tableted by a rotary tableting machine (AQUARIUS36K, Kikusui Seisakusho, Ltd.) using a 8.5 mmφ punch (tableting pressure: 8 kN, weight per tablet: 270 mg) to give core tablets.
(5) Hydroxypropylmethylcellulose (4095 g) and talc (630 g) were dissolved and dispersed in purified water (37800 g) to give dispersion liquid I. Titanium oxide (493.5 g) and iron oxide (31.5 g) were dispersed in purified water (9450 g) to give dispersion liquid II. Dispersion liquid II was added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-1200, POWREX CORPORATION) , the coating dispersion was sprayed on the core tablets obtained in (4) until the weight of the core tablet increased to 10 mg per tablet to give film-coated tablets having the following composition. Then, the film- coated tablets were dried under the reduced pressure at 40°C for 15 hr. [0079] composition of preparation. (280 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg sodium hydroxide 0.345 mg fumaric acid 1 mg hydroxypropylcellulose 2.7 mg crystalline cellulose 27 mg crospovidone 15.75 mg magnesium stearate 2.7 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 280 mg [0080] Example 4
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator
(WSG-60, POWREX CORPORATION), chlorthalidone (10750 g) , mannitol (48070 g) and crystalline cellulose (3870 g) were uniformly mixed, granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION), compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules B.
(3) Crystalline cellulose (9720 g) , crospovidone (5670 g) , magnesium stearate (972 g) , milled granules A (54430 g) and the milled granules B (26410 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules. (4) The mixed granules were tableted by a rotary tableting machine (AQUARIUS36K, Kikusui Seisakusho, Ltd.) using a 8.5 mmφ punch (tableting pressure: 8 kN, weight per tablet: 270 mg) to give core tablets. (5) Hydroxypropylmethylcellulose (4095 g) and talc (630 g) were dissolved and dispersed in purified water (37800 g) to give dispersion liquid I. Titanium oxide (493.5 g) and iron oxide (31.5 g) were dispersed in purified water (9450 g) to give dispersion liquid II. Dispersion liquid II was added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-1200, POWREX CORPORATION) , the coating dispersion was sprayed on the core tablets obtained in (4) until the weight of the core tablet increased to 10 mg per tablet to give film-coated tablets having the following composition. Then, the film- coated tablets were dried under the reduced pressure at 40°C for 15 hr. [0081] composition of preparation (280 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg sodium hydroxide 0.345 mg fumaric acid 1 mg hydroxypropylcellulose 2.7 mg crystalline cellulose 27 mg crospovidone 15.75 mg magnesium stearate 2.7 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0 . 06 mg total 280 mg
[0082] Example 5 (1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator (WSG-60, POWREX CORPORATION), chlorthalidone (5375 g) , mannitol (53450 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION), compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules B. (3) Crystalline cellulose (9720 g) , crospovidone (6075 g) , magnesium stearate (972 g) , the milled granules A (40820 g) and the milled granules B (39610 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules . (4) The mixed granules were tableted by a rotary tableting machine (AQUARIUS36K, Kikusui Seisakusho, Ltd.) using a 9.5 mmφ punch (tableting pressure: 9 kN, weight per tablet: 360 mg) to give core tablets. (5) Hydroxypropylmethylcellulose (3471 g) and talc (534 g) were dissolved and dispersed in purified water (32040 g) to give dispersion liquid I. Titanium oxide (418.3 g) and iron oxide (26.7 g) were dispersed in purified water (8010 g) to give dispersion liquid II. Dispersion liquid II was added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-1200,
POWREX CORPORATION) , the coating dispersion was sprayed on the core tablets obtained in (4) until the weight of the core tablet increased to 10 mg per tablet to give film-coated tablets having the following composition. Then, the film- coated tablets were dried under the reduced pressure at 400C for 15 hr.
[0083] composition of preparation (370 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 42.68 mg mannitol 86.93 mg crystalline cellulose 9 mg sodium hydroxide 0.69 mg fumaric acid 2 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 36 mg crospovidone 22.5 mg magnesium stearate 3.6 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 370 mg
[0084]
Example 6
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator (WSG-60, POWREX CORPORATION), chlorthalidone (5375 g) , mannitol (53450 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION) , compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules B.
(3) Crystalline cellulose (9720 g) , crospovidone (6075 g) , magnesium stearate (972 g) , the milled granules A (40820 g) and the milled granules B (39610 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules .
(4) The mixed granules were tableted by a rotary tableting machine (AQUARIUS36K, Kikusui Seisakusho, Ltd.) using a 9.5 mmφ punch (tableting pressure: 9 kN, weight per tablet: 360 mg) to give core tablets.
(5) Hydroxypropylmethylcellulose (3471 g) and talc (534 g) were dissolved and dispersed in purified water (32040 g) to give dispersion liquid I. Titanium oxide (418.3 g) and iron oxide (26.7 g) were dispersed in purified water (8010 g) to give dispersion liquid II. Dispersion liquid II was added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-1200, POWREX CORPORATION) , the coating dispersion was sprayed on the core tablets obtained in (4) until the weight of the core tablet increased to 10 mg per tablet to give film-coated tablets having the following composition. Then, the film- coated tablets were dried under the reduced pressure at 40°C for 15 hr. [0085] composition of preparation (370 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 42.68 mg mannitol 86.93 mg crystalline cellulose 9 mg sodium hydroxide 0.69 mg fumaric acid 2 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 36 mg crospovidone 22.5 mg magnesium stearate 3.6 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 370 mg
[0086]
Example 7
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator (WSG-60, POWREX CORPORATION), chlorthalidone (5375 g) , mannitol (53450 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION), compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules B.
(3) Crystalline cellulose (9720 g) , crospovidone (6480 g) , magnesium stearate (972 g) , the milled granules A (27220 g) and the milled granules B (52810 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules .
(4) The mixed granules were tableted by a rotary tableting machine (AQUARIUS36K, Kikusui Seisakusho, Ltd. ) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10 kN, weight per tablet: 540 mg) to give core tablets.
(5) Hydroxypropylmethylcellulose (4056 g) and talc (624 g) were dissolved and dispersed in purified water (37440 g) to give dispersion liquid I. Titanium oxide (488.8 g) and iron oxide (31.2 g) were dispersed in purified water (9360 g) to give dispersion liquid II. Dispersion liquid II was added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-1200, POWREX CORPORATION) , the coating dispersion was sprayed on the core tablets obtained in (4) until the weight of the core tablet increased to 20 mg per tablet to give film-coated tablets having the following composition. Then, the film- coated tablets were dried under the reduced pressure at 40°C for 15 hr. [ 0087 ] composition of preparation (560 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg hydroxypropylmethylcellulose 15.6 mg talc 2.4 mg titanium oxide 1.88 mg iron oxide 0.12 mg total 560 mg
[0088]
Example 8
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator (WSG-60, POWREX CORPORATION), chlorthalidone (10750 g) , mannitol (48070 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION), compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules B.
(3) Crystalline cellulose (9720 g) , crospovidone (6480 g) , magnesium stearate (972 g) , the milled granules A (27220 g) and the milled granules B (52810 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules .
(4) The mixed granules were tableted by a rotary tableting machine (AQUARIUS36K, Kikusui Seisakusho, Ltd. ) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10 kN, weight per tablet: 540 mg) to give core tablets.
(5) Hydroxypropylmethylcellulose (4056 g) and talc (624 g) were dissolved and dispersed in purified water (37440 g) to give dispersion liquid I. Titanium oxide (488.8 g) and iron oxide (31.2 g) were dispersed in purified water (9360 g) to give dispersion liquid II. Dispersion liquid II was added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-1200, POWREX CORPORATION) , the coating dispersion was sprayed on the core tablets obtained in (4) until the weight of the core tablet increased to 20 mg per tablet to give film-coated tablets having the following composition. Then, the film- coated tablets were dried under the reduced pressure at 400C for 15 hr. [0089] composition of preparation (560 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg hydroxypropylmethylcellulose 15.6 mg talc 2.4 mg titanium oxide 1.88 mg iron oxide 0.12 mg total 560 mg
[0090]
Example 9
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator (WSG-60, POWREX CORPORATION) , chlorthalidone (10750 g) , mannitol (48070 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules. Crystalline cellulose (7200 g) , crospovidone (3600 g) , magnesium stearate (720 g) and the milled granules (60480 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical
Machinery) to give mixed granules A. (2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION) , compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules. Crystalline cellulose (7200 g) , crospovidone (5400 g) , magnesium stearate (720 g) and the milled granules (58680 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules B. (3) The mixed granules A (180 mg) and the mixed granules B (90 mg) were tableted in the form of a bilayer by a rotary tableting machine (AQUA08242L2JI, Kikusui Seisakusho, Ltd.) using a 8.5 mmφ punch (tableting pressure: 7 kN, weight per tablet: 270 mg) to give core tablets. (4) Hydroxypropylmethylcellulose (780 g) and talc (120 g) were dissolved and dispersed in purified water (7750 g) to give dispersion liquid I. Titanium oxide (94 g) and iron oxide (6 g) were dispersed in purified water (1000 g) to give dispersion liquid II. Dispersion liquid II and purified water (250 g) were added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-650, POWREX CORPORATION), the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 10 mg per tablet to give film-coated tablets having the following composition. Then, the film-coated tablets were dried under the reduced pressure at 40°C for 15 hr. [0091] composition of preparation (280 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 18 mg crospovidone 9 mg magnesium stearate 1.8 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg sodium hydroxide 0.345 mg fumaric acid 1 mg hydroxypropylcellulose 2.7 mg crystalline cellulose 9 mg crospovidone 6.75 mg magnesium stearate 0.9 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 280 mg
[0092]
Example 10
(1) Hydroxypropylcellulose (5122 g) was dissolved in purified water (80620 g) to give liquid I. In a fluid bed granulator (WSG-60, POWREX CORPORATION), chlorthalidone (10740 g) , mannitol (48080 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules. Crystalline cellulose (7200 g) , crospovidone (3600 g) , magnesium stearate (720 g) and the milled granules (60480 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical
Machinery) to give mixed granules A. (2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION), compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules. Crystalline cellulose (7200 g) , crospovidone (5400 g) , magnesium stearate (720 g) and the milled granules (58680 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules B. (3) The mixed granules A (180 mg) and the mixed granules B (90 mg) were tableted in the form of a bilayer by a rotary tableting machine (AQUA08242L2JI, Kikusui Seisakusho, Ltd.) using a 8.5 mmφ punch (tableting pressure: 7 kN, weight per tablet: 270 mg) to give core tablets. (4) Hydroxypropylmethylcellulose (780 g) and talc (120 g) were dissolved and dispersed in purified water (7750 g) to give dispersion liquid I. Titanium oxide (94 g) and iron oxide (6 g) were dispersed in purified water (1000 g) to give dispersion liquid II. Dispersion liquid II and purified water (250 g) were added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-650, POWREX CORPORATION), the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 10 mg per tablet to give film-coated tablets having the following composition. Then, the film-coated tablets were dried under the reduced pressure at 400C for 15 hr. [0093] composition of preparation (280 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 18 mg crospovidone 9 mg magnesium stearate 1.8 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg sodium hydroxide 0.345 mg fumaric acid 1 mg hydroxypropylcellulose 2.7 mg crystalline cellulose 9 mg crospovidone 6.75 mg magnesium stearate 0.9 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 280 mg
[0094]
Example 11
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator (WSG-60, POWREX CORPORATION), chlorthalidone (5375 g) , mannitol (53450 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules. Crystalline cellulose (7200 g) , crospovidone (3600 g) , magnesium stearate (720 g) and the milled granules (60480 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical
Machinery) to give mixed granules A. (2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION), compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules. Crystalline cellulose (7200 g) , crospovidone (5400 g) , magnesium stearate (720 g) and the milled granules (58680 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules B. (3) The mixed granules A (180 mg) and the mixed granules B (360 mg) were tableted in the form of a bilayer by a rotary tableting machine (AQUA08242L2JI, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10 kN, weight per tablet: 540 mg) to give core tablets.
(4) Hydroxypropylmethylcellulose (780 g) and talc (120 g) were dissolved and dispersed in purified water (7750 g) to give dispersion liquid I. Titanium oxide (94 g) and iron oxide (6 g) were dispersed in purified water (1000 g) to give dispersion liquid II. Dispersion liquid II and purified water (250 g) were added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-650, POWREX CORPORATION), the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 20 mg per tablet to give film-coated tablets having the following composition. Then, the film-coated tablets were dried under the reduced pressure at 400C for 15 hr. [0095] composition of preparation (560 mg) chlorthalidone 12.5 mg mannitol 124.3 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 18 mg crospovidone 9 mg magnesium stearate 1.8 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 36 mg crospovidone 27 mg magnesium stearate 3.6 mg hydroxypropylmethylcellulose 15.6 mg talc 2.4 mg titanium oxide 1.88 mg iron oxide 0.12 mg total 560 mg
[0096]
Example 12
(1) Hydroxypropylcellulose (5122 g) was dissolved in purified water (80620 g) to give liquid I. In a fluid bed granulator
(WSG-60, POWREX CORPORATION), chlorthalidone (10740 g) , mannitol (48080 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules. Crystalline cellulose (7200 g) , crospovidone (3600 g) , magnesium stearate (720 g) and the milled granules (60480 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules A.
(2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION), compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained the granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules. Crystalline cellulose (7200 g) , crospovidone (5400 g) , magnesium stearate (720 g) and the milled granules (58680 g) were mixed in a tumbler mixer (TM-400S, Showa Chemical Machinery) to give mixed granules B.
(3) The mixed granules A (180 mg) and the mixed granules B (360 mg) were tableted in the form of a bilayer by a rotary tableting machine (AQUA08242L2JI, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10 kN, weight per tablet: 540 mg) to give core tablets.
(4) Hydroxypropylmethylcellulose (3900 g) and talc (600 g) were dissolved and dispersed in purified water (35000 g) to give dispersion liquid I. Titanium oxide (470 g) and iron oxide (30 g) were dispersed in purified water (10000 g) to give dispersion liquid II. Dispersion liquid II was added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-1200, POWREX CORPORATION) , the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 20 mg per tablet to give film-coated tablets having the following composition. Then, the film- coated tablets were dried under the reduced pressure at 400C for 15 hr. [0097] composition of preparation (560 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg crystalline cellulose 18 mg crospovidone 9 mg magnesium stearate 1.8 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 36 mg crospovidone 27 mg magnesium stearate 3.6 mg hydroxypropylmethylcellulose 15.6 mg talc 2.4 mg titanium oxide 1.88 mg iron oxide 0.12 mg total 560 mg
[0098]
Example 13 (1) In a fluid bed granulator (Lab-1, POWREX CORPORATION), compound A (85.36 g) , chlorthalidone (100 g) , and mannitol
(91.26 g) were uniformly mixed and granulated by spraying an aqueous solution of hydroxypropylcellulose (10.8 g) , fumaric acid (4 g) and sodium hydroxide (1.38 g) , and dried therein. The obtained granules were passed through a 16 mesh sieve
(aperture 1.0 mm) to give sieved granules. Croscarmellose sodium (23.46 g) , crystalline cellulose (30.6 g) , magnesium stearate (3.06 g) and the sieved granules (248.88 g) were mixed in a bag to give mixed granules. (2) The mixed granules were tableted by a rotary tableting machine (AQUARIUS, Kikusui Seisakusho, Ltd. ) using a 6 mmφ punch (tableting pressure: 3 KN/punch, weight per tablet: 90 mg) to give core tablets having the following composition.
Then, the core tablets were dried under the reduced pressure at 400C for 16 hr. [0099] composition of preparation (90 mg) compound A 21.34 mg chlorthalidone 25 mg mannitol 22.815 mg hydroxypropylcellulose 2.7 mg fumaric acid 1 mg sodium hydroxide 0.345 mg croscarmellose sodium 6.9 mg crystalline cellulose 9 mg magnesium stearate 0.9 mg total 90 mg
[0100]
Example 14 In a fluid bed granulator (FD-5S, POWREX CORPORATION), compound A (597.5 g) , chlorthalidone (175 g) , mannitol (2000 g) and crystalline cellulose (189 g) were uniformly mixed and granulated by spraying an aqueous solution of hydroxypropylcellulose (113.4 g) , fumaric acid (28 g) and sodium hydroxide (9.66 g) , and dried therein. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules. Crystalline cellulose (324 g) , crospovidone (216 g) , magnesium stearate (32.4 g) and the sieved granules (2668 g) were mixed in a tumbler mixer (TM-15, Showa Chemical Machinery) to give mixed granules. The mixed granules were tableted by a rotary tableting machine
(VEL50306SS2MZ, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14.8 mm, minor diameter 8 mm) (tableting pressure: 8
KN/punch, weight per tablet: 540 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 400C for 15 hr.
[0101] composition of preparation (540 mg) chlorthalidone 25 mg compound A 85.36 mg mannitol 285.66 mg crystalline cellulose 27 mg hydroxypropylcellulose 16.2 mg fumaric acid 4 mg sodium hydroxide 1.38 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg total 540 mg [0102]
Example 15
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator
(WSG-60, POWREX CORPORATION), chlorthalidone (10750 g) , mannitol (48070 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) Compound A (1024 g) , mannitol (2086 g) and crystalline cellulose (216 g) were uniformly mixed in a fluid bed granulator (FD-5S, POWREX CORPORATION) and granulated by spraying an aqueous solution of hydroxypropylcellulose (129.6 g) , fumaric acid (48 g) and sodium hydroxide (16.56 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules B.
(3) Crystalline cellulose (324 g) , crospovidone (216 g) , magnesium stearate (32.4 g) , the milled granules A (907.2 g) and the sieved granules B (1760 g) were mixed in a tumbler mixer (TM-15, Showa Chemical Machinery) to give mixed granules. The mixed granules were tableted by a rotary tableting machine (VEL50306SS2MZ, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14.8 mm, minor diameter 8 mm) (tableting pressure: 8 KN/punch, weight per tablet: 540 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 400C for 15 hr.
[0103] composition of preparation (540 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg hydroxypropylcellulose 10.8 mg fumaric acid 4 mg sodium hydroxide 1.38 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg total 540 mg [0104]
Example 16
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator
(WSG-60, POWREX CORPORATION), chlorthalidone (2688 g) , mannitol (56140 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION), compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules . A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules B. (3) Crystalline cellulose (1512 g) , crospovidone (882 g) , magnesium stearate (151.2 g) , the milled granules A (8467 g) and the milled granules B (4108 g) were mixed in a tumbler mixer (TM-60S, Showa Chemical Machinery) to give mixed granules. The mixed granules were tableted by a rotary tableting machine (COLLECT 12K, Kikusui Seisakusho, Ltd.) using a 8.5 mmφ punch (tableting pressure: 6 KN/punch, weight per tablet: 270 mg) to give core tablets. (4) Hydroxypropylmethylcellulose (390 g) and talc (60 g) were dissolved and dispersed in purified water (3850 g) to give dispersion liquid I. Titanium oxide (47 g) and iron oxide (3 g) were dispersed in purified water (500 g) to give dispersion liquid II. Dispersion liquid II and purified water (150 g) were added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-650, POWREX CORPORATION) , the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 10 mg per tablet to give film- coated tablets having the following composition. Then, the film-coated tablets were dried under the reduced pressure at
400C for 15 hr.
[0105] composition of preparation (280 mg) chlorthalidone 6.25 mg mannitol 130.55 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 21.34 mg mannitol 43.465 mg crystalline cellulose 4.5 mg hydroxypropylcellulose 2.7 mg fumaric acid 1 mg sodium hydroxide 0.345 mg crystalline cellulose 27 mg crospovidone 15.75 mg magnesium stearate 2.7 mg hydroxypropylmethylcellulose 7.8 mg talc 1.2 mg titanium oxide 0.94 mg iron oxide 0.06 mg total 280 mg
[0106]
Example 17 (1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator (WSG-60, POWREX CORPORATION), chlorthalidone (2688 g) , mannitol (5614Og) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical
Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) Sodium hydroxide (405.8 g) and fumaric acid (1176 g) were dissolved in purified water (38230 g) to give a buffer solution. Hydroxypropylcellulose (3019 g) was dissolved in purified water (47240 g) to give liquid II. In a fluid bed granulator (WSG-60, POWREX CORPORATION), compound A (20060 g) , mannitol (40860 g) and crystalline cellulose (4230 g) were uniformly mixed and granulated by spraying the buffer solution (31810 g) and further liquid II (42260 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules B. (3) Crystalline cellulose (1512 g) , crospovidone (1008 g) , magnesium stearate (151.2 g) , the milled granules A (4234 g) and the milled granules B (8215 g) were mixed in a tumbler mixer (TM-60S, Showa Chemical Machinery) to give mixed granules. The mixed granules were tableted by a rotary tableting machine (COLLECT 12K, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14 mm, minor diameter 8 mm) (tableting pressure: 10.5 KN/punch, weight per tablet: 540 mg) to give core tablets having the following composition. (4) Hydroxypropylmethylcellulose (390 g) and talc (60 g) were dissolved and dispersed in purified water (3850 g) to give dispersion liquid I. Titanium oxide (47 g) and iron oxide (3 g) were dispersed in purified water (500 g) to give dispersion liquid II. Dispersion liquid II and purified water (150 g) were added to dispersion liquid I, and the mixture was stirred to give a coating dispersion. Using a pan coating machine (DRC-650, POWREX CORPORATION) , the coating dispersion was sprayed on the core tablets obtained in (3) until the weight of the core tablet increased to 20 mg per tablet to give film- coated tablets having the following composition. Then, the film-coated tablets were dried under the reduced pressure at 40°C for 15 hr. [0107] composition of preparation (560 mg) chlorthalidone 6.25 mg mannitol 130.55 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 173.86 mg crystalline cellulose 18 mg sodium hydroxide 1.38 mg fumaric acid 4 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5 . 4 mg hydroxypropylmethylcellulose 15 . 6 mg talc 2 . 4 mg titanium oxide 1 . 88 mg iron oxide 0 . 12 mg total 560 mg [0108] Reference Example 1
In a fluid bed granulator (Lab-1, POWREX CORPORATION), compound A (42.68 g) , lactose (217.32 g) , crystalline cellulose (32 g) and monosodium fumarate (10 g) were uniformly mixed, granulated by spraying an aqueous solution of hydroxypropylcellulose (12 g) and monosodium fumarate (10 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules. The sieved granules (16.2 g) and low- substituted hydroxypropylcellulose (0.8 g) were mixed in a glass bottle to give mixed granules. The mixed granules were tableted by Autograph (manufactured by Shimadzu Corporation, AG-5000B) using a 9.5 mmφ punch (tableting pressure: 7.5 KN/punch, weight per tablet: 398.3 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 400C for 16 hr. [0109] composition of preparation (398.3 mg) compound A 50 mg lactose 254.6 mg crystalline cellulose ' 37.5 mg hydroxypropylcellulose 14.1 mg monosodium fumarate 23.4 mg low-substituted hydroxypropylcellulose 18.7 mg total 398.3 mg
[0110] Reference Example 2 In a fluid bed granulator (Lab-1, POWREX CORPORATION), compound A (42.68 g) , lactose (217.32 g) and crystalline cellulose (32 g) were uniformly mixed, granulated by spraying an aqueous solution of hydroxypropylcellulose (12 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules. The sieved granules (15.2 g) and low- substituted hydroxypropylcellulose (0.8 g) were mixed in a glass bottle to give mixed granules. The mixed granules were tableted by Autograph (manufactured by Shimadzu Corporation, AG-5000B) using a 9.5 mmφ punch (tableting pressure: 7.5 KN/punch, weight per tablet: 374.9 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 40°C for 16 hr. [0111] composition of preparation (374.9 mg) compound A 50 mg lactose 254.6 mg crystalline cellulose 37.5 mg hydroxypropylcellulose 14.1 mg low-substituted hydroxypropylcellulose 18.7 mg total 374.9 mg
[0112] Reference Example 3
In a fluid bed granulator (FD-5S, POWREX CORPORATION), compound A (597.5 g) , chlorthalidone (175 g) , mannitol (2037 g) and crystalline cellulose (189 g) were uniformly mixed, granulated by spraying an aqueous solution of hydroxypropylcellulose (113.4 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules. Crystalline cellulose (324 g) , crospovidone (216 g) , magnesium stearate (32.4 g) and the sieved granules (2668 g) were mixed in a tumbler mixer (TM-15, Showa Chemical Machinery) to give mixed granules . The mixed granules were tableted by a rotary tableting machine (VEL50306SS2MZ, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14.8 mm, minor diameter 8 mm) (tableting pressure: 8 KN/punch, weight per tablet: 540 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 40°C for 15 hr.
[0113] composition of preparation (540 mg) chlorthalidone 25 mg compound A 85.36 mg mannitol 291.04 mg crystalline cellulose 27 mg hydroxypropylcellulose 16.2 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg total 540 mg
[0114]
Reference Example 4
(1) Hydroxypropylcellulose (2800 g) was dissolved in purified water (44070 g) to give liquid I. In a fluid bed granulator
(WSG-60, POWREX CORPORATION), chlorthalidone (10750 g) , mannitol (48070 g) and crystalline cellulose (3870 g) were uniformly mixed and granulated by spraying liquid I (38870 g) , and dried to give granules. A part of the obtained granules was milled in a powermill grinder (P-7S, Showa Chemical Machinery) using a 1.5 mmφ punching screen to give milled granules A.
(2) In a fluid bed granulator (FD-5S, POWREX CORPORATION), compound A (1024 g) , mannitol (2151 g) and crystalline cellulose (216 g) were uniformly mixed, granulated by spraying an aqueous solution of hydroxypropylcellulose (129.6 g) , and dried therein to give granules. The obtained granules were passed through a 16 mesh sieve (aperture 1.0 mm) to give sieved granules B. (3) Crystalline cellulose (324 g) , crospovidone (216 g) , magnesium stearate (32.4 g) , the milled granules A (907.2 g) and the sieved granules B (1760 g) were mixed in a tumbler mixer (TM-15, Showa Chemical Machinery) to give mixed granules.
The mixed granules were tableted by a rotary tableting machine (VEL50306SS2MZ, Kikusui Seisakusho, Ltd.) using a punch (major diameter 14.8 mm, minor diameter 8 mm) (tableting pressure: 8
KN/punch, weight per tablet: 540 mg) to give core tablets having the following composition. Then, the core tablets were dried under the reduced pressure at 400C for 15 hr. [0115] composition of preparation (540 mg) chlorthalidone 25 mg mannitol 111.8 mg crystalline cellulose 9 mg hydroxypropylcellulose 5.4 mg compound A 85.36 mg mannitol 179.24 mg crystalline cellulose 18 mg hydroxypropylcellulose 10.8 mg crystalline cellulose 54 mg crospovidone 36 mg magnesium stearate 5.4 mg total 540 mg
[0116] Experimental Example 1
The dried core tablets obtained in Example 1 and Example
13 were stored in a closed glass bottle with a desiccant at
600C for 2 weeks. An increase in the amount of decomposed products was measured by the following method. Compound A was dissolved in an extract at about 1 μg/mL, and the solution was filtered using a non-aqueous filter (0.45 μm) and quantified by high performance liquid column chromatography (HPLC) under the following conditions. [0117] HPLC conditions detector: ultraviolet absorption photometer, measurement wavelength: 240 nm column: YMC-Pack ProC18, 5 μm, inner diameter: 4.6 mm, length: 150 mm column temperature: 25°C mobile phase (A): 0.05 mol/L phosphate buffer (pH 3.0) /acetonitrile mixed solution (9:1) mobile phase (B): 0.05 mol/L phosphate buffer (pH 3.0) /acetonitrile mixed solution (3:7) flow: 1 mL/min gradient program (linear) time (min) mobile phase (A) (%) mobile phase (B) (%) 0 (injecting) 100 0
10 70 30
90 ° 100
91 100 0 110 (injecting) 100 0 [0118]
The results are shown in Table 1. As shown in Table 1, by separately granulating each compound, the decomposition of compound A was suppressed. [0119] Table 1 preparation increase (%) in amount of decomposed products tablet of Example 1 2. 53 tablet of Example 13 6. 52
[0120]
Experimental Example 2 The drug dissolution property of the dried core tablets obtained in Example 14 and Reference Example 3 was evaluated by a dissolution test (0.5 w/w% dodecylsodium sulfate- containing phosphate buffer (pH 6.8, 900 mL) , Paddle Method, 50 rpm, 37°C) . The results are shown in Fig. 1, wherein -•- shows the results of the dried core tablets of Example 14 and -O- shows the results of the dried core tablets of Reference Example 3.
As shown in Fig. 1, addition of a pH control agent improved the dissolution property. [0121] Experimental Example 3
The dried core tablets obtained in Example 14 and Reference Example 3 were stored in a closed glass bottle with a desiccant at 400C for 1 month. An increase in the amount of decomposed products was measured by the following method.
Compound A was dissolved in an extract at about 1 μg/mL, and the solution was filtered using a non-aqueous filter (0.45 μm) and quantified by high performance liquid column chromatography (HPLC) under the following conditions. [0122]
HPLC conditions detector: ultraviolet absorption spectrophotometer, measurement wavelength: 240 nm column: YMC-Pack ProC18, 5 μm, inner diameter: 4.6 mm, length: 150 mm column temperature: 25°C mobile phase (A): 0.05 mol/L phosphate buffer (pH 4.0) /acetonitrile/tetrahydrofuran mixed solution (40:7:3) mobile phase (B): acetonitrile/O.05 mol/L phosphate buffer (pH 4.0) /tetrahydrofuran mixed solution (49:30:21) flow: 1 mL/min gradient program (linear)
Time (min) mobile phase (A) mobile phase
(%) (B) (%)
0 (injecting) 100 0
100 0 100
101 100 0
110 100 0
(injecting) The results are shown in Table 2. As shown in Table 2, addition of a pH control agent suppressed decomposition of compound A. [0123] Table 2 preparation increase (%) in the amount of decomposed products tablet of Example 14 0.51 tablet of Reference 1.80 Example 3 [0124] Experimental Example 4
The drug dissolution property of the dried core tablets obtained in Example 15 and Reference Example 4 was evaluated in the same manner as in Experimental Example 2. The results are shown in Fig. 2, wherein -•- shows the results of the dried core tablets of Example 15 and -O- shows the results of the dried core tablets of Reference Example 4. As shown in Fig. 2, addition of a pH control agent improved the dissolution property. [0125] Experimental Example 5
The dried core tablets obtained in Example 14 and Example 15 were stored in a closed glass bottle with a desiccant at 400C for 1 month. An increase in the amount of decomposed products was measured in the same manner as in Experimental Example 3. [0126] The results are shown in Table 3. As show in Table 3, by separately granulating each compound, the decomposition of compound A was suppressed. [0127] Table 3 preparation increase (%) in the amount of decomposed products tablet of Example 14 0. 51 tablet of Example 15 0. 31
INDUSTRIAL APPLICABILITY
[0128]
The solid preparation of the present invention is useful for the prophylaxis or treatment of circulatory diseases such as hypertension, cardiac failure, diabetic nephropathy, arteriosclerosis and the like. The solid preparation of the present invention comprising the aforementioned compound represented by the formula (I) , a pH control agent and a diuretic shows superior safety and superior dissolution property of the compound represented by the formula (I) and the diuretic.
[0129]
While some of the embodiments of the present invention have been described in detail in the above, those of ordinary skill in the art can enter various modifications and changes to the particular embodiments shown without substantially departing from the novel teaching and advantages of the present invention. Such modifications and changes are encompassed in the spirit and scope of the present invention as set forth in the appended claims .
[0130]
This application is based on US provisional application Nos. 61/085,201 and 61/085,627, the contents of which are incorporated hereinto by reference.

Claims

1. A solid preparation comprising a compound represented by the formula (I) :
wherein R1 is a monocyclic nitrogen-containing heterocyclic group having a deprotonizable hydrogen atom, R2 is an esterified carboxyl group and R3 is an optionally substituted lower alkyl, or a salt thereof, a pH control agent and a diuretic.
2. The solid preparation of claim 1, wherein the compound represented by the formula (I) or a salt thereof is (5-methyl- 2-oxo-l, 3-dioxol-4-yl)methyl 2-ethoxy-l-{ [2' - (5-oxo-4, 5- dihydro-1, 2, 4-oxadiazol-3-yl) biphenyl-4-yl] methyl} -IH- benzimidazole-7-carboxylate potassium salt.
3. The solid preparation of claim 1 or 2, wherein the diuretic is chlorthalidone or hydrochlorothiazide.
4. The solid preparation of claim 1, wherein the salt of the compound represented by the formula (I) is (5-methyl-2-oxo- 1, 3-dioxol-4-yl) methyl 2-ethoxy-l-{ [2' - (5-oxo-4, 5-dihydro- 1,2, 4-oxadiazol-3-yl) biphenyl-4-yl] methyl } -lH-benzimidazole-7- carboxylate potassium salt, and the diuretic is chlorthalidone.
5. The solid preparation of claim 1, wherein the pH control agent has pH 2 to 5.
6. The solid preparation of claim 1, wherein the pH control agent is an acidic substance selected from the group consisting of tartaric acid, citric acid, lactic acid, fumaric acid, succinic acid, phosphoric acid, malic acid, ascorbic acid, acetic acid and acidic amino acid, or a salt thereof, or a solvate thereof.
7. The solid preparation of claim 1, wherein the pH control agent is monosodium fumarate, or a combination of fumaric acid and sodium ion donor.
8. A solid preparation comprising a first part comprising a compound represented by the formula (I) :
wherein R1 is a monocyclic nitrogen-containing heterocyclic group having a deprotonizable hydrogen atom, R2 is an esterified carboxyl group and R3 is an optionally substituted lower alkyl, or a salt thereof and a pH control agent, and a second part comprising a diuretic, which is obtained by granulating separately from the first part.
9. The solid preparation of claim 1, wherein the compound represented by the formula (I), or a salt thereof and the pH control agent are contained in a first part and the diuretic is contained in a second part, which is a multi-layer tablet comprising a first layer comprised of the first part and a second layer comprised of the second part.
10. The solid preparation of claim 1, wherein the pH control agent is in a proportion of 0.01-20 wt% of the preparation.
11. A method of stabilizing a compound represented by the formula (I) or a salt thereof and a diuretic in a- solid preparation, which comprises adding a pH control agent to the solid preparation.
12. A method of improving dissolution property of a compound represented by the formula (I) or a salt thereof from a solid preparation comprising the compound or the salt thereof and a diuretic, which comprises adding a pH control agent to the solid preparation.
EP09788017.3A 2008-07-31 2009-07-29 Solid pharmaceutical composition Active EP2310385B1 (en)

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Families Citing this family (6)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
TW201014850A (en) 2008-09-25 2010-04-16 Takeda Pharmaceutical Solid pharmaceutical composition
US9387249B2 (en) 2008-12-23 2016-07-12 Takeda Pharmaceutical Company Limited Methods of treating hypertension with at least one angiotensin II receptor blocker and chlorthalidone
CN102351853B (en) * 2011-08-29 2014-03-12 石药集团欧意药业有限公司 Azilsartan medoxomil compound, preparation method and medicinal composition thereof
JP2015526477A (en) * 2012-08-22 2015-09-10 ゼノポート,インコーポレイティド Oral dosage form of methylhydrogen fumarate and its prodrug
JP6935301B2 (en) * 2016-11-18 2021-09-15 花王株式会社 Coated particles for monohalogenoamine production
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Family Cites Families (28)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US4444769A (en) * 1982-07-27 1984-04-24 Mylan Pharmaceuticals, Inc. Antihypertensive diuretic combination composition and associated method
IL102183A (en) 1991-06-27 1999-11-30 Takeda Chemical Industries Ltd Biphenyl substituted heterocyclic compounds their production and pharmaceutical compositions comprising them
CA2125251C (en) 1993-06-07 2005-04-26 Yoshiyuki Inada A pharmaceutical composition for angiotensin ii-mediated diseases
US5721263A (en) 1993-06-07 1998-02-24 Takeda Chemical Industries, Ltd. Pharmaceutical composition for angiotensin II-mediated diseases
JP3057471B2 (en) 1993-06-07 2000-06-26 武田薬品工業株式会社 Agent for preventing or treating angiotensin II-mediated diseases
EP1258254A4 (en) 2000-02-21 2004-02-04 Takeda Chemical Industries Ltd SLOW-RELEASE PREPARATIONS CONTAINING A PHYSIOLOGICALLY ACTIVE COMPOUND, NOT SO SOLUBLE IN WATER, AND METHOD OF PRODUCING AND USING THE SAME
JP2001294524A (en) 2000-04-12 2001-10-23 Taisho Pharmaceut Co Ltd Oral solid preparation containing acetaminophen
FR2812876B1 (en) 2000-08-08 2002-09-27 Galderma Res & Dev NOVEL BIAROMATIC COMPOUNDS THAT ACTIVATE PPAR-GAMMA TYPE RECEPTORS AND THEIR USE IN COSMETIC OR PHARMACEUTICAL COMPOSITIONS
CN1293867C (en) * 2001-05-25 2007-01-10 爱诗爱诗制药株式会社 Drug preparations
WO2003047573A1 (en) 2001-12-03 2003-06-12 Takeda Chemical Industries, Ltd. Insulin resistance improving agents
DE10244681A1 (en) 2002-09-24 2004-04-08 Boehringer Ingelheim International Gmbh New solid telmisartan-containing pharmaceutical formulations and their preparation
CA2532450C (en) 2003-07-16 2012-09-11 Boehringer Ingelheim International Gmbh Chlorthalidone combinations
US7157584B2 (en) * 2004-02-25 2007-01-02 Takeda Pharmaceutical Company Limited Benzimidazole derivative and use thereof
US7625940B2 (en) 2005-07-01 2009-12-01 Accu-Break Technologies, Inc. Method of treating hypertension with a very low dose of chlorthalidone
KR20070053239A (en) 2004-09-06 2007-05-23 코와 가부시키가이샤 Glomerular Disease Therapeutics
US20070049636A1 (en) 2005-08-26 2007-03-01 Joerg Rosenberg Pharmaceutical compositions
US20060159747A1 (en) 2004-12-17 2006-07-20 Boehringer Ingelheim International Gmbh Telmisartan and hydrochlorothiazide combination therapy
WO2006063737A1 (en) * 2004-12-17 2006-06-22 Boehringer Ingelheim International Gmbh Combination therapy comprising telmisartan and hydrochlorothiazide
JP4795362B2 (en) 2005-03-30 2011-10-19 武田薬品工業株式会社 Benzimidazole derivatives and uses thereof
JP2008540573A (en) 2005-05-13 2008-11-20 マイクロビア インコーポレーテッド 4-Bialyl-1-phenylazetidin-2-ones
WO2006132440A1 (en) * 2005-06-09 2006-12-14 Takeda Pharmaceutical Company Limited Solid preparation
EP2058010B1 (en) 2006-08-10 2012-05-02 Takeda Pharmaceutical Company Limited Pharmaceutical composition
WO2008045006A1 (en) 2006-10-11 2008-04-17 Fako Ilaclari A. S. Formulations of candesartan
WO2008068217A2 (en) 2006-12-04 2008-06-12 Boehringer Ingelheim International Gmbh Pharmaceutical composition comprising a coated hmg-coa reductase inhibitor and an inhibitor of the renin-angiotensin system
EA016593B1 (en) 2007-03-28 2012-06-29 Такеда Фармасьютикал Компани Лимитед Solid pharmaceutical composition comprising a benzimidazole-7-carboxylate derivative and a ph control agent
CA2705625A1 (en) 2007-08-01 2009-02-05 Teva Pharmaceutical Industries Ltd. Improved formulations of candesartan
WO2009058950A2 (en) 2007-10-30 2009-05-07 Dr. Reddy's Laboratories Ltd. Pharmaceutical formulations comprising telmisartan and hydrochlorothiazide
US9387249B2 (en) 2008-12-23 2016-07-12 Takeda Pharmaceutical Company Limited Methods of treating hypertension with at least one angiotensin II receptor blocker and chlorthalidone

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
See references of WO2010013835A2 *

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ECSP11010856A (en) 2011-03-31
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PE20110551A1 (en) 2011-09-02
WO2010013835A2 (en) 2010-02-04
AU2009277455A1 (en) 2010-02-04
CR20110111A (en) 2011-04-28
CO6341633A2 (en) 2011-11-21
PT2310385T (en) 2017-09-11
DOP2011000032A (en) 2011-02-28
CN102164918B (en) 2014-05-07
MA32553B1 (en) 2011-08-01
UY32017A (en) 2010-02-26
ZA201100871B (en) 2012-05-30
CN102164918A (en) 2011-08-24
JP5635491B2 (en) 2014-12-03
MX2011001150A (en) 2011-03-29
TW201008915A (en) 2010-03-01
US20110123615A1 (en) 2011-05-26
IL210819A0 (en) 2011-04-28
BRPI0916847A2 (en) 2016-02-10
WO2010013835A3 (en) 2010-06-10
GEP20146062B (en) 2014-03-25
AR072883A1 (en) 2010-09-29
JP2011529444A (en) 2011-12-08
EA201170273A1 (en) 2011-08-30
CA2732018A1 (en) 2010-02-04
EP2310385B1 (en) 2017-06-07
US9169238B2 (en) 2015-10-27
NZ590948A (en) 2012-06-29

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